procedure man tb

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For decades now, tuberculosis (TB) has been a major public health hazard contributing to theconsiderable loss of productive man-hours. Hence, controlling TB to a level where it is no longer apublic health problem is a priority under the Health Sector Reform Agenda. This, in turn, is envisionedto contribute significantly to the poverty reduction efforts of the government.

Successful TB control depends largely on the capacity of various health care facilities toadminister TB management based on technically sound, evidence-based, and consistent policies andprocedures. Adopting standardized TB management protocols and guidelines facilitates effective programimplementation in all parts of the country. Hence, Executive Order No. 187, series of 2003, institutionalizedthe Comprehensive and Unified Policy for Tuberculosis.

The National Tuberculosis Control Program (NTP) Manual of Procedures (MOP) is decidedlya milestone in the implementation of standardized management protocols and guidelines for all healthcare facilities in the country involved in TB cure and prevention. This revised version (4th edition) of theMOP embodies new strategies and initiatives designed to contribute to national targets of 70-per-centcase detection and 85-per-cent cure rate. Among these initiatives are: a) collaboration with key partnersthrough installation of Public-Private Mix DOTS (PPMD) units; b) expansion of DOTS services to coverother health –related sectors like teachers and school personnel, the military, and those in prisons; c)shift from single-dose to fixed-dose combination anti-TB drugs, which aims for improved treatmentcompliance and better logistics management; d) adoption of a quality assurance system for more reliablesputum microscopy; e) strengthening of TB Diagnostic Committees to support the management of lessinfectious cases; and f) adoption of policy statements governing monitoring, supervision, and evaluation,as well as advocacy activities on TB cure and prevention.

The MOP has undergone a series of revisions involving partners/implementers as externalreviewers and sources of critical technical and editorial inputs. The NTP is extremely grateful to all thosewho contributed to the development and revision of the MOP, which aims to contribute to more effectiveways of implementing the NTP throughout the Philippines. For their technical expertise and financialassistance in making this product a success, acknowledgment goes to the following: The Global Fundto fight AIDS, Tuberculosis and Malaria (GFATM); Japan International Cooperation Agency (JICA);Local Enhancement and Development for Health Project – Management Sciences for Health (LEAD-MSH); Medicos Del Mundo (MDM); Philippine Coalition Against Tuberculosis (PhilCAT); PhilippineTuberculosis Initiatives in the Private Sector (PhilTIPS); Tropical Disease Foundation, Incorporated(TDFI); United States Agency for International Development (USAID); World Health Organization (WHO);and World Vision Development Foundation, Incorporated (WVDFI).

We hope that the MOP will be a tool for unifying our efforts towards the attainment of our visionof a TB-free Philippines.

HON. FRANCISCO T. DUQUE III, MD, MSc.Secretary of Health

Department of Health December 2005Republic of the Philippines

Foreword

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A publication of the Department of Health (DOH), Government of the Philippines, in cooperation with

the following local and international key stakeholders and partners:

Board of Advisers:

1. Dr. Myrna Cabotaje, NCDPC, DOH

2. Dr. Jaime Lagahid, IDO, DOH

3. Dr. Jennifer Ann Mendoza-WI, PhilCAT

Publications Staff

1. Dr. Ma. Theresa Velasco, Technical Editor

2. Ms. Laila Garcia, Assistant Technical Editor

3. Ms. Rose Gonzales, Creative Director

Technical Working Group (TWG)

Department of Health

1. Dr. Anna Marie Celina Garfin, NCDPC

2. Dr. Ernesto Bontuyan Jr., NCDPC

3. Ms. Agnes del Rosario, NCDPC

4. Mr. Ferdinand La Puebla, NCDPC

5. Ms. Ellen Melia Castillo, NTRL

6. Ms. Edna Nito, NCHP

Centers for Health Development

1. Dr. Lydia Rogando, CHD–Bicol

2. Dr. Flor Elona, CHD–Eastern Visayas

3. Dr. Willie Cabauatan, CHD–Cagayan Valley

4. Ms. Joy Tabotabo, CHD–Central Visayas

5. Ms. Gemma Tan, CHD–Ilocos

Local Government Units

1. Dr. Niela Jorvina, Laguna Provincial Health Office

2. Dr. Christina Giango, Cebu Provincial Health Office

3. Ms. Evangeline Rambuyon , Negros Provincial Health Office

4. Ms. Letty Rivera, Batangas Provincial Health Office

Partners

1. Dr. Michael Voniatis, WHO

2. Dr. Tomohiro Shirahama, JICA

3. Dr. Arthur Lagos, JICA

4. Dr. Marilyn Gorra, PhilTIPS

5. Dr. Charles Yu, PhilTIPS

6. Mr. Jose Ibarra Angeles, PhilTIPS

7. Ms. Elaine Umali, WVDFI

Technical Review Panel (TRP)


1. Dr. Rosalind Vianzon, NCDPC

2. Ms. Cirila Negad, NCDPC

3. Ms. Arlene Rivera, NCDPC

4. Dr. Vivian Lofranco, LCP

5. Dr. Nora Cruz, NTRL

6. Ms. Paz Rostrata, NTRL

Centers for Health Development

1. Dr. Sylvia Somontan, CHD–Caraga

2. Dr. Eloisa Segura, CHD–Davao

3. Dr. Amelia Medina, CHD–NCR

4. Dr. Edith Caloyloy, CHD–Western Visayas

5. Ms. Marilou Gecosala, CHD–Northern Mindanao

Local Government Units

1. Dr. Bernard Caspe, Iloilo City Health Office

2. Dr. Ma. Lourdes San Juan, Pasay City Health Office

3. Dr. Marian Isiderio, Eastern Samar Provincial Health Office

4. Ms. Teresita Puente, Pasig City Health Office

5. Ms. Myla Espino, Pasig City Health Office

6. Ms. May Fernando, Bulacan Provincial Health Office

Partners

1. Dr. Mariquita Mantala, LEAD for Health Project

2. Dr. Jubert Benedicto, PhilCAT

3. Ms. Amelia Sarmiento, PhilCAT

4. Mr. Albert Angelo Concepcion, PhilCAT

5. Dr. Maria Rubio, MDM

6. Dr. Jose Luis Portrero, MDM

7. Dr. Ma. Imelda Quelapio, TDFI/GFATM

8. Dr. Melvin Magno, WVDFI

Credit Page

FOREWORD i

CREDIT PAGE ii

MANUAL OUTLINE iii

LIST OF ACRONYMS v

LIST OF TABLES viii

LIST OF FIGURES ix

GLOSSARY x

CHAPTER I INTRODUCTION

Prevalence of TB In the Country 1

History of TB Control in the Philippines 2

Vision, Mission, and Goal of the NTP 9

NTP Objectives and Strategies 9

Roles of Collaborating Agencies 11

Functions of Health Workers 13

CHAPTER II CASE FINDING

I. Objective 18

II. Definition of Terms 18

III. Policies 18

IV. Procedures 19

V. Quality Assurance for DSSM 27

CHAPTER III CASE HOLDING

I. Objective 28

II. Definition of Terms 28

III. Policies 31

IV. Procedures 35

V. Treatment Outcome 50

VI. Summary Guide 50

CHAPTER IV RECORDING AND REPORTING

I. Objective 53

II. Policies 53

III. NTP Recording Forms 54

IV. Persons Responsible for the Recording Forms 73

V. NTP Reporting Forms 74

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Manual Outline

CHAPTER V LOGISTICS MANAGEMENT

I. Product Selection 82

II. Procurement 83

III. Distribution and Storage 83

IV. Rationale Use, Monitoring, and Evaluation 85

CHAPTER VI MONITORING, SUPERVISION, AND EVALUATION

I. Objective 90

II. Policies 91

III. Procedures 92

IV. Monitoring Forms 94

CHAPTER VII OVERVIEW OF THE HEALTH PROMOTION

PROGRAM FOR THE NTP 101

ANNEXES

1 Guidelines for Implementing Tuberculosis 105

Control Program in Children (AO No. 178 Series of 2004)

2 Sample Packages of FDCs & SDFs 115

3 The TB Diagnostic Committee (TBDC) 117

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AFB Acid Fast Bacilli

BCG Bacille Calmette-Guerin

BFAD Bureau of Food and Drug

BHS Barangay Health Station

BHW Barangay Health Worker

CDR Case Detection Rate

CHD Center for Health Development

CHO City Health Officer or City Health Office

CIDA Canadian International Development Agency

Collaboration in Rural and Urban Sites to Halt Tuberculosis

CUP Comprehensive and Unified Policy for TB Control in the Philippines

CXR Chest X-ray

DILG Department of Interior and Local Government

DOH Department of Health

DOT Directly Observed Treatment

DOTS Directly Observed Treatment, Short Course

DRS Drug Resistance Survey

DSSM Direct Sputum Smear Microscopy

E Ethambutol

EP Extra pulmonary Tuberculosis

EPI Expanded Program for Immunization

EQA External Quality Assessment

FDC Fixed Dose Combination

FEFO First Expiry, First Out

FHSIS Field Health Services Information System

FM Family Member

GDF Global Drug Facility

GFATM Global Fund to Fight AIDS, Tuberculosis, and Malaria

H Isoniazid

List of Acronyms

CRUSH TB

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HSRA Health Sector Reform Agenda

IEC Information, Education and Communication

JICA Japan International Cooperation Agency

LCE Local Chief Executive

LCP Lung Center of the Philippines

LGU Local Government Unit

MC Memorandum Circular

MDR-TB Multiple Drug Resistant TB

MHC Main Health Center

MHO Municipal Health Officer

MOP Manual of Procedures

MT Medical Technologist

National Coordinating Committee for PPMD

NCDPC National Center for Disease Prevention and Control

NCHP National Center for Health Promotion

NGO Non-Government Organization

NHIP National Health Insurance Program

NIT National Institute of Tuberculosis

NPS National TB Prevalence Survey

NTP National Tuberculosis Control Program

NTRL National Tuberculosis Reference Laboratory

OIF Oil Immersion Field

PAS Para-Amino Salicylate

PCCP Philippine College of Chest Physicians

PD Presidential Decree

PhilCAT Philippine Coalition Against Tuberculosis

PHO Provincial Health Office

PMA Philippine Medical Association

PPMD Public-Private Mix DOTS

PSMID Philippine Society for Microbiology and Infectious Disease

PTB Pulmonary Tuberculosis

PTSI Philippine Tuberculosis Society, Inc.

NCC-PPMD

QA Quality Assurance

QC Quality Control

QI Quality Improvement

R Rifampicin

RA Republic Act

RAD Return After Default

Regional Coordinating Committee for PPMD

RHM Rural Health Midwife

RHU Rural Health Unit

S Streptomycin

SCC Short Course Chemotherapy

SDF Single Drug Formulation

TB Tuberculosis

TBCS TB Control Service

TBDC Tuberculosis Diagnostic Committee

TCL Target Client List

UNICEF United Nations Children’s Fund

USAID United States Agency for International Development

UST University of Santo Tomas

WB World Bank

WHO World Health Organization

WPRO Western Pacific Regional Office

Z Pyrazinamide

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RCC-PPMD

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Table 1.1 Comparative Data between 1981-1983 NPS and 1997 NPS

Table 3.1 Classification of TB Cases

Table 3.2 Types of TB Cases

Table 3.3 Recommended Category of Treatment Regimen

Table 3.4 Treatment Regimen for Categories I & III: 2HRZE/4HR (FDC)

Table 3.5 Treatment Regimen for Category II: 2HRZES/HRZE/5HRE (FDC)

Table 3.6 Treatment Regimen for Categories I & III: 2HRZE/4HR (SDF)

Table 3.7 Treatment Regimen for Category II: 2HRZES/HRZE/5HRE (SDF)

Table 3.8 Drug Dosage per KG Body Weight

Table 3.9 Schedule of DSSM Follow-up for Categories I and III

Table 3.9.a Schedule of DSSM Follow-up for Category II

Table 3.10 Treatment Modifications for New PTB Smear-Positive Cases Based on the Resultsof DSSM Follow-up for Category I Treatment Regimen Without Extension

Table 3.10.a Treatment Modifications for New PTB Smear-Positive Cases Based on Results ofDSSM Follow-up for Category I Treatment Regimen With Extension

Table 3.10.b Treatment Modifications for PTB Smear-Positive Cases Based on the Results of DSSMFollow-up for Category II Treatment Regimen Without Extension

Table 3.10.c Treatment Modifications for PTB Smear-Positive Cases Based on DSSM Follow-upResults for Category II Treatment Regimen With Extension

Table 3.11 Guide in Managing Adverse Reactions to Anti-TB Drugs

Table 3.12 Treatment Modifications for New Smear-Positive Cases Who Interrupted Treatment

Table 3.12.a Treatment Modifications for Relapse and Treatment Failure Cases Who InterruptedTreatment

Table 4.1 Persons Responsible for the Recording Forms

Table 5.1 Computation for Quarterly Drug Requirement for Stop TB Kits

Table 5.2 Computation for Quarterly FDC BP Drug Requirement

Table 5.3.a Computation for Quarterly SDF BP Drug Requirement

Table 5.3.b Computation for Quarterly SDF Tablets Drug Requirement

Table 5.4 Computation for Annual Estimated Supplies for DSSM

Table 5.5 Computation for Annual Estimated Recording and Reporting Forms

Table 6.1 Program Indicators

Table 7.1 Health Promotion Activities for Addressig Various Tasks

List of Tables

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Figure 1.1 Flow of NTP Activities

Figure 2.1 Flow Chart for the Diagnosis of Pulmonary TB

Figure 2.2 Flow Chart for the Diagnosis of Smear-Negative Pulmonary TB

Figure 2.3 Guide to Case Finding

Figure 2.4 Guide to Diagnosis and Initiation of Treatment

Figure 3.1 Category I Treatment Modification Based on DSSM Follow-up Results

Figure 3.2 Category II Treatment Modification Based on DSSM Follow-up Results

Figure 3.3 Category III Treatment Modification Based on DSSM Follow-up Results

Figure 3.4 Guide to Case Holding

Figure 3.5 Guide to Ensuring Treatment

Figure 5.1 Anti-TB Drug Management Cycle

Figure 6.1 Flow of Reporting

List of Figures

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Active Case Finding Purposive effort by a health worker to find TB cases from among TBsymptomatics in the community who do not consult in a DOTS facility

Communicating with other people to gain their support for an issueand influence their behavior in a specified way

An activity to discover or find TB cases

An activity to treat TB cases through proper treatment regimen andhealth education

It is a continuous and sustained process of educating the people forthem to understand and develop their critical consciousness of theirexisting conditions. It entails organizing the people to work collectivelyand efficiently on their immediate and long-term problems andmobilizing people to develop their capability and readiness to respondto and take action on their immediate/long-term needs.

Number of new smear-positive pulmonary TB cases registered in aspecified period who were cured divided by the total number of newsmear-positive pulmonary TB cases registered in the same periodmultiplied by 100.

Directly Observed Treatment [A trained DOTS facility worker (ortreatment partner) personally observes the smear-positive patienttake anti-TB medicines everyday during the whole course of treatment.]

Directly Observed Treatment Short-Course (A comprehensive strategyto control TB). The five components of DOTS are:1. Government commitment to ensuring sustained, comprehensive

TB control activities;2. Case detection by DSSM among symptomatic patients self-

reporting to health services (passive case finding);3. Standard short-course chemotherapy using regimens of six to

eight months, for at least all confirmed smear-positivecases; complete drug taking through DOT supervised by DOTSfacility workers during the whole course of treatment for all smear-positive cases;

4. A regular, uninterrupted supply of all essential anti-tuberculosisdrugs and other materials; and

5. A standard recording and reporting system that allows assessmentof case finding and treatment results for each patient and of thetuberculosis control program’s overall performance.

Any facility providing DOTS services; includes BHS/BHC, RHU/MHC,PPMD unit, hospital-based DOTS facility, and DOTS implementingunits, e.g., prisons, schools, HMOs, military facilities, etc.

Advocacy

Case Finding

Case Holding

Community Organizing

Cure Rate

DOT

DOTS

DOTS Facility

Glossary

The part of health care that is concerned with promoting healthbehavior (It helps people understand their behavior and how it affectstheir health. It also encourages behavior that promotes health,prevents illness, cures disease, and facilitates rehabilitation. It isalso a process by which individuals and groups of people learn tobehave in a manner conducive to promotion, maintenance, orrestoration of health.)

A process of enabling people to take action to improve health (It isneeded in order to build health public policy, create supportiveenvironment, develop personal skills, reorient health services, andstrengthen community action.)

What people do in order to maintain health and/or return to health,ranging from individual behavior to collective behavior; includes whatis done and why it is done (It concerns specific steps taken; it issometimes called hierarchy of resort.)

A process of generating information or release of ready-madeinformation or prototypes, as well as distribution through all selectedchannels of communication

A condition which is resistant against at least Isoniazid and Rifampicin

A process of linking up with individuals, groups, and institutions onthe basis of a common objective

Finding a case of tuberculosis from among TB symptomatics whopresent themselves at the DOTS facility

Over-all in charge of running and operating the DOTS facility for theprivate-initiated PPMD; includes rural health physicians, municipalhealth officers, and hospital-based physicians

The act of pledging or giving an obligation among Local ChiefExecutives, such as Governors, Mayors, and other governmentofficials

Person responsible for coordinating DOTS activities for the private-initiated PPMD

Private facility, with private referring physicians, providing DOTSservices

Public facility, with private referring physicians, providing DOTSservices

Groups of people who provide support or sustain one another bydiscussing common problems, such as tuberculosis, alcoholism, etc.

When a DSSM has all three negative results

When a DSSM has at least two positive results

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Private-Initiated PPMD

Information, Educationand Communication (IEC)

MDR-TB

Health Education

Health Promotion

Health-seeking Behavior

Networking

Passive Case Finding

Political Commitment

Public-Initiated PPMD

PPMD Coordinator

Physician

Sectoral Support

Smear-Positive

Smear-Negative

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An adaptation of commercial marketing, sales concepts, and techniquesto the attainment of social goals (It seeks to make health-relatedinformation products easily available and affordable to low-incomepopulations and those at risk while promoting the adoption of healthybehavior.)

A process of engaging people in action, redirecting existing or creatingnew resources to achieve a society’s or a community’s social goals (Itimplies wide-scale participation. It is also a process of bringing togetherall feasible and practical inter-sectoral and social allies to raise people’sawareness of the demand for a particular development program, toassist in the delivery of resources and services, and to strengthencommunity participation for sustainability and self-reliance.)

DSSM done for TB symptomatics to establish a diagnosis of TB (Threesputum specimens should be collected.)

DSSM done to monitor the sputum status of a patient after treatmentis initiated (Only one sputum specimen is collected, preferably the earlymorning phlegm.)

Material from the respiratory tract brought out by coughing (This materialis used for DSSM.)

A brand name for DOH’s re-energized fight against TB (It is a systematicand nationwide movement spearheaded by DOH to control TB. It isconsidered the official communication handle of NTP.)

Any person exhibiting symptoms or signs suggestive of tuberculosis, inparticular cough of long duration (two or more weeks), and with orwithout one or more of the following symptoms: fever; chest and/or backpains not referable to any musculo-skeletal disprders; hemoptysis orrecurrent blood-streaked sputum; significant weight loss; and othersymptoms, such as sweating, fatigue, body malaise, and shortness ofbreath

Mycobacterium tuberculosis that causes tuberculosis (It is acid-faststained with Ziel-Nielsen staining method.)

Note: The definitions in this section apply only to the terms’ usage in this Manual of Procedures.

Social Mobilization

Sputum Microscopy forDiagnosis

Sputum Microscopy forFollow-up

Sputum Specimen

TB Network

TB Symptomatic

Tubercle Bacillus

Social Marketing

PREVALENCE OF TB IN THE COUNTRY

Tuberculosis (TB) has been a major public health problem in the Philippines for the past several

decades. Research has shown that while TB is curable, the disease adversely affects a large segment

of the population, particularly the economically productive sector. The causal agent, Mycobacterium

tuberculosis, is easily transmitted through airborne droplet nuclei when patients with pulmonary TB

cough or sneeze. If left untreated, TB could lead to a disabling condition and even death. Also, partial

treatment of cases may cause drug resistance that could lead to non-cure.

In 2002, TB was the sixth among the 10 leading causes of death and the 10 leading causes of

illness in the country. While the mortality rate from TB has decreased in the past 20 years (from 206

deaths per 100,000 population in 1982 to 36 deaths per 100,000 in 2002), still around 75 Filipinos die

of TB everyday. Globally, the Philippines is one of 22 countries identified by the World Health Organization

(WHO) as having a high burden of TB, ranking at ninth worldwide. It ranks third in terms of new smear-

positive TB notification rate in the WHO-Western Pacific Region (WHO Report 2003).

Comparative data gathered from two National Tuberculosis Prevalence Surveys (1981-1983

and 1997) reflect an encouraging trend in TB control in the country, although the changes have not been

dramatically significant (Table 1.1). The annual risk of TB infection, or the probability of a child getting

infected with TB within a year, declined very slightly in 15 years, from 2.5 per cent in 1982 to 2.3 per

cent in 1997. This measure is generally accepted as a sensitive indicator. The percentage of the

population afflicted with TB decreased from 6.6/1,000 in 1981-1983 to 3.1/1,000 in 1997. The prevalence

of culture-positive cases likewise declined very slightly from 8.6/1,000 to 8.1/1,000. Percentage of

radiographic findings suggestive of TB has remained the same at 4.2% in the 15 years between the two

surveys. The 1997 NPS also revealed that TB cases were about three times more common among

males than females and most of these cases were in the 30- to 59-year-old age bracket representing

the economically productive age group in the country.

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Table 1.1. Comparative Data between 1981-1983 NPS and 1997 NPS

1981-1983 1997

1. Annual risk of TB infection 2.5% 2.3%

2. Prevalence of sputum smear-positive cases 6.6/1,000 3.1/1,000

3. Prevalence of culture-positive cases 8.6/1,000 8.1/1,000

4. Radiographic findings suggestive of TB 4.2% 4.2%

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HISTORY OF TB CONTROL IN THE PHILIPPINES

The Beginnings

TB control efforts in the Philippines reflect a continuous struggle to curb the spread of a curable

but highly infectious disease with great implications on the nation’s productivity.

The earliest organized initiative on TB control in the Philippines can be traced to a private

organization, the Philippine Islands Anti-Tuberculosis (precursor of the Philippine Tuberculosis Society,

Inc. or PTSI), way back in 1910. The Society put up a TB hospital in Quezon City; this was later re-named

Quezon Institute after President Manuel L. Quezon, who was afflicted with the disease. The period 1910-

1929 was largely devoted to case finding and in-patient services at a time when the only treatment

regimen available consisted of bed rest, isolation, or hospitalization.

The 1930s and 1940s witnessed a more organized approach to TB control in the wake of the

increasing incidence of TB cases in the country. The TB Commission under the Philippine Health Service

was established in 1932 through Republic Act (RA) 3743. The Bureau of Health took over the powers

and duties of the TB Commission in 1933. More laws were later enacted to bolster the anti-TB initiatives.

RA 4130 (Sweepstakes Law) established the Philippine Charity Sweepstakes Office (PCSO) primarily

to raise funds to support PTSI’s operations. Most notable among PCSO’s initial achievements were the

setting up of Chest Clinics in selected areas of the country and acceleration of in-patient activities.

From the ‘50s onward, dramatic strides in TB cure have been taken worldwide. Streptomycin

injection was first used as part of TB treatment in 1949. With assistance from the United Nations Children’s

Fund (UNICEF), the BCG vaccination program was introduced in the Philippines between 1951 and 1952

as a preventive measure against TB. Triple therapy, consisting of the anti-TB drugs Isoniazid (INH), Para-

amino salicylate (PAS), and streptomycin, was initiated in 1954.

Organizational changes to step up the TB control program were also effected in the ‘50s and

‘60s. In 1950, the TB Commission evolved into the Division of Tuberculosis under the supervision of the

Secretary of Health. The Division in turn established the TB Center at the DOH Compound and collaborated

with the TB Ward of San Lazaro Hospital. The move allowed for expanded services, which included chest

x-ray, sputum and bronchial washing examinations, and case holding. Treatment at that time consisted

of streptomycin injection plus oral PAS tablets.

Congress passed RA 1136 (Tuberculosis Law) in 1954. This became the basis for the creation

of both the Division of Tuberculosis under an appointed Director and the National Tuberculosis Center

of the Philippines (NTCP) established at the DOH Compound. The NTP received a boost from RA 1136

with the provision of funds to support its operations.

The first ever TB prevalence survey, the Minglanilla Prevalence Survey, was conducted in 1964

in Cebu province. Survey results placed the prevalence of smear-positive cases at 4/1,000. During this

period, Quezon Institute was operating at its largest bed capacity at 1,350 beds.

Expansion of the TB Control Program

The late ‘60s through to the mid-‘70s witnessed a vigorous nationwide expansion of the TB

program through accelerated and expanded control activities at the rural health units (RHUs), which

were established under RA 1086. The strengthened RHUs increasingly took on greater responsibility

for TB control efforts. PTSI launched the domiciliary care program in 1973, a move which eventually

led to the reduction of Quezon Institute’s bed capacity to 700. As the new TB Control Program was

implemented in all RHUs, the admissions at Quezon Institute began to be limited only to the seriously

ill cases.

It was also in 1973 that the Philippine College of Chest Physicians (PCCP) was formed as an

accredited non-government organization (NGO) society of the Philippine Medical Association (PMA)

with TB as one of its initial primary concerns. The partnership between DOH and PTSI was intensified

as the two organizations defined, complemented, and supported each other’s roles in TB control. The

new thrust emphasized the following: 1) importance of BCG vaccination; 2) case finding through sputum

microscopy; and 3) case holding/treatment through domiciliary means.

The partnership likewise paved the way for the establishment of the National Institute of

Tuberculosis (NIT) in 1976, with support from WHO and UNICEF. NIT focused on human resource

development, in the process carrying out operational researches and providing training to local and

foreign health workers on TB control using the primary health care approach. The year was also

highlighted by the issuance of a Presidential Decree (PD) requiring compulsory BCG vaccination, which

became a prime component of the Expanded Program for Immunization (EPI). Two years later, in 1978,

PTSI adopted the NTP policies and guidelines in its catchment areas.

Nearly two decades after the Minglanilla survey, NIT conducted the first National TB Prevalence

Survey (NPS) in 1982-1983, with assistance from WHO and UNICEF. Another significant development

during this period was the establishment of the Lung Center of the Philippines (LCP) as a tertiary hospital.

LCP became a referral center for pulmonary cases, including TB.

Contemporary Milestones

The ‘80s through to the ‘90s and the beginning years of the new millennium witnessed the

implementation of significant organizational and technical strategies that further strengthened TB control

efforts in the Philippines. This was also the time when the NTP Manual of Procedures was developed

and revised.

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Organizational Strategies

The reorganization of the Department of Health after the People Power revolution in 1986,

through Executive Order 119, paved the way for the establishment of the TB Control Service (TBCS)

under the Office for Public Health Services. A year later, the Strengthened National TB Control Program

was launched. Under this program, the TBCS was given a P200-million budget for drugs.

The NTP got a big boost in 1990 with the financial and technical support from the Italian

government and World Bank (WB) under the five-year Philippine Health Development Project.

In the early 1990s, the Local Government Code of 1991 paved the way for the devolution of

health services, including delivery of TB services, from DOH to the LGUs. While DOH remained at the

helm of policy development, regulation, and provision of technical and financial assistance, the LGUs

managed the TB program and delivered their services to their constituents through the RHUs and the

Barangay Health Stations (BHSs).

A showcase of this new health service delivery paradigm was the TB control project in Cebu.

The Cebu project, with technical and financial support from JICA, tested the WHO-recommended policies

and guidelines, improved laboratory facilities with the establishment of the Regional TB Laboratory in

Cebu City and upgrading of microscopy centers, and systematized TB data collection and recording.

A council created in 1993 by PCCP to act as its working arm for TB successfully released in

1994 a set of algorithms on the diagnosis and treatment of TB. An external evaluation of the NTP done

in 1993 noted that while case-finding activities improved tremendously, problems in case holding persisted.

In 1995, the TBCS issued through Administrative Order No. 1-A series of 1995 the revised policies and

guidelines on the diagnosis and management of TB which, in essence, adopted the WHO-recommended

policies. The thrust adopted by NTP was to improve case holding activities.

The forging of partnerships and active interactions among the various sectors engaged in the

fight against TB became more evident in the ‘90s. The Philippine Coalition Against Tuberculosis (PhilCAT)

was organized in 1994 to serve as coordinating body for the various government and non-government

agencies, private groups, academe, and other concerned institutions involved in TB control. The

organizations that banded to form PhilCAT include PCCP, DOH, Philippine Society for Microbiology and

Infectious Disease (PSMID), PTSI, Cure TB, and the American College of Chest Physicians-Philippine

Chapter.

The joint advocacy of these organizations was largely responsible for the issuance of Proclamation

No. 840 issued by the President of the Philippines in 1996. The proclamation declared August 19 of

every year as the National TB Day. March 24, on the other hand, is observed as World TB Day. On both

occasions, DOH, in collaboration with PhilCAT and other partners, conducts activities that would draw

public attention to the organized fight against TB.

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In September 1998, the NTP became one of the DOH flagship programs. Memorandum Circular

(MC) No. 98-155 issued by the President, then concurrent secretary of the Department of Interior and

Local Government (DILG), pronounced the TB Control Program as the highest priority health program

of the LGUs and prescribed the DOTS strategy.

The Health Sector Reform Agenda (HSRA) adopted by DOH in 1999 made the National TB

Control Program one of the top priorities among the public health programs. The organizational reforms

under the HSRA led to the clustering of various public health programs, merging of offices, and significant

reduction in manpower, all designed to improve delivery of health services. The following specific

objectives of the HSRA were likewise seen to impact positively on the TB sector:

• To secure funding for priority public health programs;

• To promote the development of local health systems and to ensure their effective performance;

• To provide fiscal autonomy to government hospitals;

• To strengthen the capacities of health regulatory agencies; and

• To expand the coverage of the National Health Insurance Program (NHIP).

Technical Strategies

In 1986, a new treatment regimen was introduced in the National TB Control Program -- the

Short-Course Chemotherapy (SCC), which highlighted use of Rifampicin, 2HRZ/4HR. During this period,

a fourth drug – streptomycin or ethambutol – was also being used for the intensive phase of treatment

regimen at the Quezon Institute for confined or in-patients. The SCC was adopted nationwide in 1987.

To ensure treatment compliance, the various drugs were packaged in blister-packs, an innovative strategy

that was later adopted by neighboring countries.

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Over the years, greater compliance with the NTP through a standard national policy to guide

all stakeholders has been perceived as a pressing need. The Comprehensive and Unified Policy (CUP)

for Tuberculosis Control in the Philippines was developed jointly by DOH and PhilCAT in 2003. As

specified in Executive Order No. 187 series of 2003, the CUP is an instrument to harmonize and unify

TB control efforts in the Philippines in the public and private sectors. The CUP, among other provisions,

emphasizes the adoption of the NTP’s DOTS (Directly Observed Treatment, Short Course) strategy.

Implementation of the DOTS strategy goes back to the mid-1990s when an intensified national

campaign to increase awareness about TB and to mobilize support for its prevention and control was

launched. In 1995, the TB Clinic of the University of Santo Tomas (UST) initiated the use of DOTS in

managing its out-patient TB cases. DOH piloted the DOTS strategy in three areas in 1996 through the

CRUSH TB (Collaboration in Rural and Urban Sites to Halt Tuberculosis) project. DOTS was pilot-tested

in Iloilo City, Antique, and Batangas. Results from this project became the basis for expansion of the

new NTP to other areas and made possible the subsequent nationwide implementation of DOTS.

The NTP officially adopted DOTS strategy with the issuance of Administrative Order No. 24

series of 1996. DOTS implementation hinges on five components: 1) political commitment; 2) diagnosis

by sputum microscopy; 3) Directly Observed Treatment (DOT), i.e., supervised treatment; 4) uninterrupted

drug supply; and 5) standardized recording and reporting.

DOTS was subsequently replicated in 30 areas in 1997-1998 and in all public-sector health

facilities in the country by 2001. DOTS expansion was facilitated by the active participation of LGUs,

the implementation of DOTS with BHWs as treatment partners, and the support from various international

agencies, such as WHO, WB, JICA, World Vision-Canadian International Development Agency (CIDA),

Australian Aid (AusAID), and Medicos del Mundo. It has also gained access to international resources,

such as the Global Drug Facility (GDF) and Global Fund on AIDS, TB and Malaria (GFATM), to augment

supply of anti-TB drugs in the country.

The second NPS was conducted in 1997. In 1999, a new consensus on TB diagnosis, treatment,

and control was forged through a consultative process coordinated by PSMID, PCCP, and DOH under

the auspices of PhilCAT.

Initiatives to strengthen the NTP included delivery of quality DOTS services through expansion

of DOTS implementation in all government health facilities. The National TB Reference Laboratory

(NTRL) was established in 2002 to improve quality assurance of microscopy through the established

network of microscopy facilities. It is also spearheading the national drug resistance survey (DRS).

The NTRL also spearheads the implementation of the External Quality Assessment (EQA)

nationwide. The EQA refers to a system of periodic independent measurement of performance through

collaboration with another competent laboratory; it aims to maintain high quality results from the microscopy

centers.

To improve the quality of diagnosis among sputum smear-negatives with chest x-ray findings

suggestive of PTB, the NTP initiated the creation of TB Diagnostic Committees. The TBDCs are

established at the provincial and city levels to review the sputum smear-negatives with chest x-ray

findings suggestive of PTB. The TBDC is chaired by the NTP medical coordinator, with members from

both the public and private sectors. TB experts, who represent various disciplines, also sit on the

committee. The TBDC evaluates, by consensus, the appropriate recommendations for quality patient

management. (Refer to Annex 3 for more information on the TBDC.)

By the end of 2002, public sector DOTS coverage has reached almost 100 per cent. Despite

this achievement, case detection rate (CDR) has remained below the 70-per-cent target. It was learned

from the 1997 NPS and other local studies that a significant number of TB cases sought care from the

private sector. In this context and within the DOTS expansion strategy, DOH adopted in 2003 the national

strategy of Public-Private Mix DOTS (PPMD).

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The PPMD is a strategy designed to increase case detection and to synchronize the management

of TB both in the public and private sectors. A PPMD unit can be public- or private-initiated depending

on where DOTS service provision is offered. In a public-initiated PPMD unit, DOTS services are centered

in a public DOTS facility with the private physicians referring patients for services. In a private-initiated

PPMD, the operations and management of DOTS services are centered on a privately owned and

managed DOTS facility. Whether public- or private-initiated, PPMD units implement DOTS in consonance

with the approved operational policies, standards, and technical guidelines of the NTP (Refer to

Operational Guidelines for Public—Private Mix DOTS in the Philippines, DOH and PhilCAT, 2004).

With PhilCATS’ support, the strategy was implemented to further mobilize private sector

physicians, professional societies and academicians, and other NGOs. In addition, additional resources

were secured for PPMD implementation through international donors.

Certification of DOTS facilities is an initiative to ensure that quality DOTS is implemented in

both public and private facilities. Guided by the Sentrong Sigla framework, it provides an assurance to

health seekers from the public and private sectors that a TB DOTS Center is capable of providing safe

and effective DOTS services. Moreover, certification ensures standardization of the provision of DOTS

services through a uniform set of standards. DOTS certification is a prerequisite to PhilHealth accreditation

and a means for the facility to avail itself of the PhilHealth TB outpatient benefit package.

In 2003, the NTP also started the shift from single dose formulation (SDF) to fixed dose

combination (FDC) drugs. This simplifies treatment, prevents development of drug resistance, and

ensures regular and complete drug delivery to DOTS centers. The NTP is also upgrading the various

CHD TB Reference Centers to improve its microscopy component.

Another milestone in the NTP, DOTCh (DOT in Children), was piloted in three areas between

2002 and 2005. The pilot phase paved the way for testing the guidelines developed by the Task Force

for TB in Children composed of experts from the public and private sectors. (Details about the strategy

may be found in Annex 1: Administrative Order 178).

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Development of the NTP Manual of Procedures

The NTP Manual of Procedures (MOP) is the basis for NTP implementation in all DOTS facilities.

Early development of the NTP Manual of Procedures dates back from 1969 however, the first

NTP Manual of Procedures (MOP) was developed in 1980. This MOP highlighted the use of sputum

microscopy as the primary diagnosis tool and the introduction of the Standard Drug Regimen for TB

treatment.

In 1988, the first MOP was revised. This 2nd edition presented the results of the 1981- 1983

First National TB Prevalence Survey (NPS). This also marked the adoption of the Short Course

Chemotherapy (SCC) for the management of TB cases under the NTP.

In 1997, the Technical Guidelines of the New TB Control Program was developed by the

Department of Health (DOH), in collaboration with DOH-JICA (Japan International Cooperation Agency)

Public Health Development Project and the WHO Western Pacific Regional Office (WPRO), in accordance

to the recommendations from the external evaluation conducted by WHO in 1993. This document

emphasized on D.O.T.S. (Directly Observed Treatment-Short Course) or “Tutok Gamutan” as the NTP’s

core framework for a nationwide TB control strategy. Subsequently, the start of rapid expansion of DOTS

in the country in 1997 embodied, as well, the implementation of this material/document.

The NTP Manual of Procedures (MOP) 3rd edition was written in 2001. The change from the

previous Technical Guidelines reflected that the publication was useful, not only for training , but also

in providing instructions or procedures to all health personnels in their delivery of TB services. This MOP

also served as a vital tool in the orientation/training of the private sector and other government agencies

in their implementation of NTP-DOTS.

In 2004, the Department of Health initiated the fourth revision of the MOP in the light of current

initiatives and policy changes in the NTP. These initiatives included the use of fixed dose combination

anti-TB drugs, EQA, adoption of the Public-Private Mix DOTS, strengthening of the TB Diagnostic

Committees, DOTS facility certification and accreditation, and development of the health promotion plan

specific to TB. Thus, with all these developments, it is but rational for the NTP to recast the MOP into

its current presentation.

VISION, MISSION, AND GOAL OF THE NTP

Vision: A country where TB is no longer a public health problem

Mission: Ensure that TB DOTS services are available, accessible, and affordable to the communities

in collaboration with the LGUs and other partners

Goal: To reduce prevalence and mortality from TB by half by the year 2015 (Millennium

Development Goals)

TARGETS:

1. Cure at least 85 per cent of the new sputum smear-positive TB cases discovered

2. Detect at least 70 per cent of the estimated new sputum smear-positive TB cases

NTP OBJECTIVES AND STRATEGIES

The NTP’s four-pronged set of objectives calls for improvement of access to and quality of

services, enhancement of patients’ health-seeking behavior, sustainability of support for TB control

activities, and strengthening management of TB control services at all levels.

Objective A:

Improve access to and quality of services provided to TB patients, TB

symptomatics, and communities by health care facilities and providers

Strategies:

1. Enhance quality of TB diagnosis.

• Adopt quality assurance system for direct sputum smear examination, including external

quality assurance.

• Establish more TB Diagnostic Committees and expand their functions to include TB in

children

• Strengthen the network of quality laboratory services in accordance with NTRL

roles/functions.

2. Ensure TB patients’ treatment compliance.

• Implement an efficient drug supply management system.

• Adopt directly observed treatment (DOT) through treatment partners.

3. Ensure public and private health care providers’ adherence to the implementation of national

standards of care for TB patients.

• Establish and sustain public-private mix DOTS, including the public-public mix DOTS.

• Expand hospital-based DOTS.

• Advocate for the widespread adoption of a comprehensive and unified policy on TB.

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4. Improve access to services through innovative service delivery mechanisms for patients living in

challenging areas (geographically isolated communities, with peace and order problem, culturally-

different, and those in institutions like prisons).

Objective B:

Enhance the health-seeking behavior on TB by communities, especially the TB symptomatics

Strategies:

1. Develop effective, appropriate, and culturally-responsive IEC/ communication materials.

2. Organize barangay advocacy groups.

Objective C:

Increase and sustain support and financing for TB control activities

Strategies:

1. Facilitate implementation of TB-DOTS facilities certification and accreditation.

2. Build TB coalitions among different sectors.

3. Advocate for counterpart input from local government units.

4. Mobilize/extend other resources to address program limitations.

Objective D:

Strengthen management (technical and operational) of TB control services at all levels.

Strategies:

1. Enhance managerial capability of all NTP program managers at all levels.

2. Establish an efficient data management system for both public and private sectors.

3. Implement a standardized recording and reporting system.

4. Conduct regular monitoring and evaluation at all levels.

5. Advocate for political support through effective local governance.

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ROLES OF COLLABORATING AGENCIES


1. Formulate plans, policies, and standards.

2. Advocate for political commitment and awareness of TB control in the community.

3. Oversee program implementation in coordination with the LGUs.

4. Provide logistics assistance in terms of:

• Anti-TB drugs;

• Laboratory supplies;

• Prototypes of educational materials; and

• NTP recording and reporting forms.

5. Provide technical assistance, including training of LGU staff.

6. Monitor and evaluate regularly NTP activities, including Quality Assurance System and TBDC

implementation/operation.

7. Collate and analyze data from all reports and feedback findings and recommendations to LGU staff

concerned.

8. Collaborate with PhilCAT, NGOs, and the private sector to promote and implement the PPMD

strategy.

9. Initiate, through the CHDs, DOTS certification at the regional level.

10. Implement hospital-based DOTS for DOH-retained hospitals.

11. Together with the National Center for Health Promotion, orchestrate the development of

information/education/communication (IEC) materials.

International Partners

1. Provide technical assistance in the development or revision of policies, guidelines and standards.

2. Provide financial support to augment the fund gap of the NTP.

3. Participate in key activities of the NTP such as monitoring and evaluation.

4. Participate as technical advisors in the existing organizational structures of the NTP as necessary.

Local Government Units (LGUs)

1. Develop local policies and work for passage of resolutions on program implementation.

2. Develop a local plan on TB control, in consultation with DOH/CHD and other stakeholders.

3. Designate a Provincial/City Medical NTP Coordinator and/or other staff, such as nurses and medical

technologists.

4. Assign the NTP Medical and Nurse Coordinators as the Chairperson and Secretariat of the TBDC,

respectively.

5. Ensure the presence of physicians, nurses, midwives, and community volunteers at the municipal-

level facility.

6. Implement the plan and provide resources for the following:

• Monitoring/supervision/evaluation;

• Capability building;

• Drugs for Category 3 patients and SDF for patients who develop adverse drug reactions;

• Augmentation of laboratory supplies

• NTP reporting forms, referral forms, laboratory request forms;

• TBDC activities;

• Local IEC materials;

• Manpower; and

• Quality assurance activities.

7. Evaluate and monitor implementation of plan.

8. Implement hospital-based DOTS and referral system in LGU hospitals.

9. Prepare, analyze, and submit quarterly reports.

10. Implement External Quality Assurance for laboratory.

11. Plan, initiate, and implement PPMD activities in accordance with the National Strategy on PPMD.

PhilCAT and Other Private Partners

1. Participate in the formulation of plans, policies, guidelines, and standards.

2. Advocate DOTS in the private sector.

3. Participate in the initiation and implementation of PPMD through the following activities:

• Advocacy;

• Training;

• Monitoring and evaluation;

• Development of advocacy materials; and

• Operations research.

4. Assist in mobilization and management of resources, including human resources, in the

establishment of PPMD.

5. Participate in certification of private DOTS facilities.

Multi-sectoral Agencies

1. National Coordinating Committee for PPMD (NCC-PPMD)

The function of the NCC-PPMD is to discuss and resolve administrative and technical issues related

to PPMD implementation, in cooperation with the RCC-PPMD. These involve:

a. Policy development for Implementation of PPMD;

b. Technical advice to the RCC-PPMD;

c. Monitoring and supervision of PPMD units; and

d. Ensuring availability, adequacy, and regularity of drug supply.

2. Regional Coordinating Committee for PPMD (RCC-PPMD)

The function of the RCC-PPMD, in coordination with the National Coordinating Committee (NCC-

PPMD), is to discuss and resolve managerial and technical issues related to launching and

implementing PPMD units at the regional level. These involve:

a. Technical advice to PPMD Units;

b. Trainings and advocacy activities;

c. Monitoring and supervision of PPMD units;

d. Ensuring availability, adequacy, and regularity of drug supply; and

e. Participation in DOTS certification.

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FUNCTIONS OF HEALTH WORKERS

DOH - NTP Staff

1. Develop national policies and plans.

2. Allocate budget for program implementation, including logistics.

3. Promote advocacy activities to foster political commitment and community awareness.

4. Exercise overall coordination among all NTP stakeholders.

5. Coordinate logistics management.

6. Provide NTP drugs and laboratory supplies.

7. Provide regular technical assistance to CHDs and LGUs, specifically in the areas of training,

monitoring, supervision, and evaluation.

8. Collate and analyze Quarterly Reports for planning and policy development.

9. Set standards for DOTS certification.

10. Conduct operational research on TB.

CHD NTP Coordinators (Physician/Nurse/MT)

1. Develop Work and Financial Plan at CHD level.

2. Promote advocacy activities to foster political commitment at the LGU level, as well as community

awareness.

3. Exercise overall coordination among all NTP stakeholders at the regional level.

4. Ensure adequacy of NTP drugs and supplies at the local level.

5. Provide regular technical assistance in the areas of training and planning.

6. Monitor and evaluate the implementation of NTP and recommend remedial measures to each LGU.

7. Collate and analyze NTP reports for planning purposes.

8. Submit regularly all consolidated Quarterly Reports to DOH (Central).

National TB Reference Laboratory (NTRL) Staff

1. Develop a national plan and policies for NTP laboratory management.

2. Develop and oversee implementation of QA system nationwide.

3. Carry out capability building measures in partnership with the CHDs.

4. Conduct monitoring and supervision in coordination with the CHDs.

5. Provide technical assistance to regional laboratories and to private laboratories engaged with the

NTP, e.g. PTSI.

6. Monitor drug resistance level.

7. Perform EQA to the microscopy centers of CHD-NCR 4A and 4B.

Regional TB Reference Laboratory

1. Oversee the implementation of the NTP’s External Quality Assurance System (EQA) on microscopy

at the regional level.

2. Provide technical assistance to the QA centers and microscopy centers.

3. Develop laboratory management plan on NTP to be integrated with the respective CHD NTP plans.

4. Conduct monitoring, supervision and evaluation of QA centers and microscopy centers on a regular

basis.

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Provincial/City NTP Coordinators (Physician/Nurse/MT)

1. Organize provincial planning, budgeting, and evaluation activities.

2. Implement advocacy activities to generate political commitment and community awareness.

3. Coordinate all NTP activities within the province/city.

4. Ensure availability and adequacy of NTP supplies. Manage drug and laboratory supply system.

5. Conduct trainings to ensure success of program implementation.

6. Monitor, supervise, and evaluate the implementation of NTP and QA and execute corrective or

remedial measures.

7. Collate and analyze quarterly reports of all DOTS facilities.

8. Consolidate all quarterly reports and submit these to CHD NTP coordinator.

9. Implement QA for quality laboratory work at all DOTS facilities.

10. Mobilize resources for TBDC and serve as chairperson/s of the TBDC (NTP medical coordinator).

Serve as secretariat (NTP nurse-coordinator).

11. Assess and refer chronic TB cases to higher level of care.

Physicians

1. Organize planning and evaluation of NTP activities in DOTS facilities.

2. Utilize available resources in the area for TB control activities.

3. Supervise health staff to ensure proper implementation of NTP policies, such as:

a. Identification, examination, and classification of TB cases;

b. Implementation of case holding mechanisms, such as DOT;

c. Analysis and submission of quarterly reports to the PHO/CHO;

d. Referral of TB cases to the TB Diagnostic Committee or other health facilities,if needed;

e. Ensuring proper procedure in the collection and transport of sputum specimen to microscopy

center; and

f. Ensuring adequacy of NTP drugs and supplies.

4. Attend to all diagnosed TB cases for clinical assessment, prescription of appropriate treatment

regimen, and management of adverse drug reactions, if any.

5. Provide continuous health education to all TB patients placed under treatment and encourage family

and community participation in TB control.

6. Coordinate with local chief executives (LCEs) to ensure funds and personnel for program

implementation.

Nurses

1. Together with other NTP staff / workers, manage the procedures for case-finding activities.

2. Open the NTP treatment card.

3. Assign and supervise a treatment partner for patient who will undergo DOTS.

4. Supervise rural health midwives (RHMs) to ensure proper implementation of DOTS.

5. Maintain and update the TB Register.

6. Facilitate requisition and distribution of drugs and other NTP supplies.

7. Provide continuous health education to all TB patients placed under treatment and encourage family

and community participation in TB control.

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8. In coordination with the physician, conduct training of health workers.

9. Prepare, analyze, and submit the quarterly reports to PHO/ CHO.

Midwives

1. Together with other health staff, implement the following case-finding activities:

a. Identify TB symptomatics and collect sputum specimens for microscopy.

b. Refer all diagnosed TB cases to physician or nurse for clinical evaluation and initiation of

treatment.

c. Maintain and update NTP Treatment Cards. (Use of TB Symptomatics Masterlist/ TB Symptomatics

Target Client List is optional).

2. Implement DOT with treatment partners.

a. Provide continuous health education to all TB patients placed under treatment and encourage

family and community participation in TB control activities.

b. Conduct regular consultation meetings (preferably weekly) with the assistance of the physician

or nurse during the course of treatment.

c. Collect sputum specimen for follow-up examination on the scheduled date/s during the

course of treatment.

d. Report and retrieve defaulters within two (2) days.

e. Refer patients with adverse drug reactions to physician for further evaluation and management.

f. Supervise and instruct community health volunteers who would be the treatment partners to

ensure proper implementation of DOT.

Medical Technologists or Microscopists*

1. Do DSSM for diagnosis and follow-up.

2. Inform the physician, nurse, or midwife of the DSSM result.

3. Maintain and update the NTP Laboratory Register.

4. Prepare quarterly report on laboratory activities and submit this to the physician or nurse.

5. Prepare and submit the quarterly laboratory supplies requirement to the physician.

6. Store sputum smears to allow sampling by the provincial or city NTP coordinator for blinded

re-checking as part of the External Quality Assessment.

* Microscopists are medical or paramedical regular staff of the DOTS facility that is trained to do basic sputum microscopy.

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Barangay Health Workers (BHWs) and other community health volunteers are key players in the

implementation of DOTS.

1. Refer TB symptomatics to the DOTS facility for sputum collection.

2. Implement DOT, together with the health personnel.

3. Keep and update the NTP ID Cards.

4. Report and retrieve defaulters within two (2) days.

5. Attend regular consultation meetings with the health personnel, together with the patient and

treatment partner.

6. Refer patients with adverse reactions, if any, to the health personnel.

7. Provide health education to the patient, family members, and the community.

Hospital-based NTP Coordinators

1. Coordinate all NTP activities in the hospital with the assistance of the CHD and Provincial NTP

coordinators.

2. Supervise hospital NTP health workers to ensure proper implementation of the following NTP

policies:

a. Identification and examination of TB symptomatics with DSSM;

b. Implementation of DOT for identified cases;

c. Ensuring availability and adequacy of anti-TB drugs and supplies;

d. Referral of patients to RHU/MHC for continuation of treatment

(NTP Referral Form should be properly filled out by physician or nurse.); and

e. Provision of continuous health education to all patients placed under DOT.

3. Encourage patient’s family members to participate in TB control activities.

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Barangay Health Workers (BHWs) and other Community Health Volunteers

Figure 1.1. Flow of NTP Activities

Symptoms of TBCough for two or more weeks, with or without:• Fever• Chest and/or back pains not referable to any

musculo-skeletal disorders• Hemoptysis or recurrent blood-streaked sputum• Significant weight loss• Other symptoms, such as sweating, fatigue, body malaise, shortness of

breath

Sputum specimens (3 specimens) with NTP Laboratory Request Formfor Direct Sputum Smear Microscopy

Diagnosis

Case Finding

Initiation of Treatment

(Results of the DSSM. If results are Smear negative and with chestx-ray suggestive of TB, refer to TBDC for evaluation. )

Case Holding with DOTS Sputum specimen (1 specimen) with LaboratoryRequest Form for DSSM

Treatment Completion

Report Treatment Outcome / Request Supplies

Monitoring and Supervision

COMMUNITY

DOTS FACILITY

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TBDC

MICROSCOPY CENTER

MICROSCOPY CENTER

Results (DSSM for follow-up)

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Case Finding

Case finding, which is the identification and diagnosis of TB cases among individuals with

suspected signs and symptoms of TB, is a basic step in TB control. Fundamental to case finding is the

detection of infectious cases through direct sputum smear microscopy (DSSM). DSSM is the principal

diagnostic method adopted by the NTP because:

1. It provides a definitive diagnosis of active TB;

2. The procedure is simple;

3. It is economical; and

4. A microscopy center could be put up even in remote areas.

DSSM results serve as bases for categorizing TB symptomatics according to standard case

definition. These are also used to: a) monitor progress of patients with sputum smear-positive TB while

they are receiving anti–TB treatment; and b) confirm cure at the end of treatment.

I. OBJECTIVE

Early identification and diagnosis of TB cases

II. DEFINITION OF TERMS

TB symptomatic – any person with cough for two or more weeks with or without the

following symptoms: fever; chest and/or back pains not referable to any musculo-skeletal disorders;

hemoptysis or recurrent blood-streaked sputum; significant weight loss; and other symptoms, such

as sweating, fatigue, body malaise, shortness of breath

Active case finding – a health worker’s purposive effort to find TB cases (among TB

symptomatics in the community) who do not consult with personnel in a DOTS facility

Passive case finding – finding TB cases among TB symptomatics who present themselves

in a DOTS facility

III. POLICIES

1. DSSM shall be the primary diagnostic tool in NTP case finding.

2. All TB symptomatics identified shall be asked to undergo DSSM for diagnosis before start of

treatment, regardless of whether or not they have available X-ray results or whether or not they

are suspected of having extra-pulmonary TB. The only contraindication for sputum collection

is hemoptysis; in which case, DSSM will be requested after control of hemoptysis.

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3. Pulmonary TB symptomatics shall be asked to undergo other diagnostic tests (X-ray and/or

culture), if necessary, only after they have undergone DSSM for diagnosis with three sputum

specimens yielding negative results. The TBDC will evaluate the results of the chest X-ray,

together with the clinical history and findings, and will recommend whether or not the case will

be started on treatment.

4. Since DSSM is the primary diagnostic tool, no TB diagnosis shall be made based on the results

of X-ray examinations alone. Likewise, results of the skin test for TB infection (PPD skin test)

should not be used as bases for TB diagnosis in adults.

5. All municipal and city health offices shall be encouraged to establish and maintain at least one

sputum microscopy unit in their areas of jurisdiction.

6. Private-initiated Public-Private Mix DOTS (PPMD) units shall each have an in-house microscopy

service.

7. Passive case finding shall be implemented in all DOTS facilities. Concomitant active case

finding shall be encouraged only in areas where a cure rate of 85 per cent or higher has been

achieved, or in areas where no sputum-smear positive case has been reported in the last three

months.

8. Only trained medical technologists or microscopists shall perform DSSM (smearing, fixing, and

staining of sputum specimens, as well as reading, recording, and reporting of results). However,

in far flung areas, BHWs or other community health volunteers may be allowed to do smearing

and fixing of specimens, as long as they have been trained and are supervised by their respective

NTP medical technologists/microscopists.

IV. PROCEDURES

A. Identification of TB Symptomatics

(To be accomplished by DOTS facility staff)

1. Identify TB symptomatics consulting at the DOTS facility. Look out for those having cough

for two or more weeks, with or without one or more of the following signs and symptoms:

a. fever;

b. chest and/or back pains not referable to any musculo-skeletal disorders;

c. hemoptysis or recurrent blood-streaked sputum;

d. significant weight loss; and

e. other symptoms, such as sweating, fatigue, body malaise, and shortness of breath.

2. Motivate TB symptomatic to undergo DSSM. Explain importance of the procedure and

that of submitting three sputum specimens. Obtaining results from three sputum specimens

increases the probability of finding acid fast bacilli.

3. Record details of each specimen submission (name of TB symptomatic, date of submission,

and result) in the TB Symptomatics Masterlist/TB Symptomatics Target Client List.

4. Encourage household members of identified TB cases, who are also TB symptomatics,

to undergo DSSM.

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B. Collection and Transport of Sputum Specimens to the Microscopy Center


1. Explain the importance of submitting three sputum specimens taken within two days.

a. First specimen, also referred to as spot specimen, is collected at the time of consultation,

or as soon as the TB symptomatic is identified.

b. Second specimen is the very first sputum produced early in the morning immediately after

waking up. It is collected by the patient according to instructions given by the DOTS facility

staff.

c. Third specimen, or second spot specimen, is collected when the TB symptomatic comes

back to the DOTS facility to submit the second specimen.

d. All specimens should be collected according to instructions given by the DOTS facility

staff. The first and third specimen collections are supervised by the DOTS facility staff to

ensure quality sputum specimen collection. If quality sputum is not collected within two

days, the patient is given one week to complete the three-specimen collection. If the patient

fails to complete the three-specimen collection within one week, another set of three should

be collected.

2. Prepare sputum cup and request form. Label body of sputum cup, indicating patient’s complete

name, and order of specimen (1st, 2nd, or 3rd).

3. Demonstrate how to produce quality sputum. Advise patient to:

a. Rinse his/her mouth with water.

b. Breathe deeply, hold breath, then exhale slowly. Repeat the entire sequence twice.

c. Cough strongly at the height of deep inspiration after inhaling deeply for the third time, and

spit the sputum in the container.

Observe precautions against infection during the demonstration. Stay behind the patient.

Collect specimen outside the DOTS facility where aerosols containing TB bacilli are diluted and

sterilized by direct sunlight.

4. Collect specimen and check quantity and quality of sputum.

5. Seal sputum specimen container, pack it securely, and transport it to a microscopy center or

laboratory, together with the completely filled up NTP Laboratory Request Form for DSSM. Do

this as soon as possible or within four days after collection.

6. If specimen cannot be sent to a microscopy unit early enough, store it in a cool, dark, and safe

place. No specimen shall remain unexamined over the weekend.

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C. Smearing, Fixing, and Staining of Sputum Specimen and Reading, Recording, and Reporting

of Results

(To be accomplished by medical technologist or microscopist)

1. Record the information in the NTP Laboratory Register, including the type of sputum specimen

submitted, i.e., mucoid, purulent, blood-streaked, or salivary.

2. Smear, fix, and stain each slide.

3. Read each slide and interpret the result as follows:

0- No AFB seen in 300 oil immersion field (OIF)

+n – 1-9 AFB seen in 100 OIF

1+ - 10 – 99 AFB seen in 100 OIF

2+ - 1-10AFB /OIF in at least 50 fields

3 + -more than 10 AFB/OIF in at least 20 fields

4. Interpret the results of the three specimens and write the final laboratory diagnosis in the lower

portion of the NTP Laboratory Request Form for DSSM and on the Remarks column of the

NTP Laboratory Register. Laboratory diagnoses are classified as follows:

a. Smear-positive - at least two positive sputum smear results

b. Doubtful - only one positive out of three sputum specimens examined (Request for another

set of three sputum specimens).

• If at least one specimen from the second set of specimens is positive, laboratory

diagnosis is positive.

• If all three specimens from the second set of specimens are negative, laboratory

diagnosis is negative.

c. Smear-negative - all three sputum smear results negative

5. Send request form back to requesting unit.

D. Decision on Patient’s Diagnosis Based on Laboratory Results


1. Inform patient of result.

• If positive, refer patient to physician for assessment and initiation of treatment; and,

• Encourage household members with signs and symptoms of TB to consult at DOTS facility.

• If doubtful, ask patient to submit another three sputum specimens within one week.

• If negative, refer patient to physician for further assessment.

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E. Diagnosis of Smear-negative Patients with Persistent Symptoms

(To be accomplished by physician)

1. Re-assess smear-negative patients with persistent symptoms of TB. (Refer to Flow Chart 2.1

& 2.2)

2. Refer patient for X-ray examination, if warranted.

3. If X-ray findings are suggestive of TB, refer patient to the TBDC. In areas where there is no

TBDC, physician may manage the patient.

F. Referral to TBDC

(To be accomplished by physician)

1. Fill up TBDC Referral Form and send it to TBDC, together with all available chest X-ray films.

2. Wait for TBDC evaluation of results, which is sent back to the DOTS facility.

3. Carry out TBDC recommendations.

For detailed information about TBDC, refer to Annex 2.

G. Summary of Procedure

The following four flow charts summarize the procedure for TB case finding:

1. Flow Chart for the Diagnosis of Pulmonary Tuberculosis;

2. Flow Chart for the Diagnosis of Smear-Negative Pulmonary Tuberculosis;

3. Guide to Case Finding; and

4. Guide to Diagnosis and Initiation of Treatment.

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23

Figure 2.1. Flow Chart for the Diagnosis of Pulmonary TB

TB Symptomatic(cough for 2 weeks or more)

Three (3) sputum collection

A. 2 or 3 Smear-Positive B. Only one (1) Smear-Positive

Classify asSmear-Positive TB

Collect another 3 SputumSpecimens Inmmediately

If at least one (1) Smear-Positive If all Smear-Negative

Classify as smear-Positive TB Request for CXR

If consistent with active TB If not consistent with active TB

Classify as smear-positive TB

Observation/further exam.,If necessary

C. All 3 Smear-Negative

Refer to Physician(Observe him/her with

SymptomaticTreatment for 2 or 3 weeks)

If symptoms persist,request for CXR

(Refer to the flow charton the next page.)

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Figure 2.2. Flow Chart for the Diagnosis of Smear-Negative Pulmonary TB

This flow chart assists the physicians in making a decision for smear-negatives.

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Classify asSmear-

Negative TB

C. All 3 Smear-Negative

Refer to Physician(Symptomatic Tx for 2-3 wks)

If symptoms persist, request for CXR

Consistentwith active TB

NotConsistent

with active TB

Observation/further exam.

Abnormalfindings on

CXR

No Abnormalfindings on

CXR

TB DiagnosticCommittee

Observation/further exam.

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

jica

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Figure 2.3. Guide to Case Finding

SPUTUM COLLECTION UNIT(To be accomplished by DOTS facility staff)

1. (Optional) Register patient in TB Symptomatics Masterlist (or TB Symptomatics TargetClient List) (see Chapter IV, p. 54).

2. Explain the importance of three sputum collections to the TB symptomatics.

3. Label each sputum container (name and order no.1,2,3).

4. Collect three quality sputum specimens (1st spot, early morning, 2nd spot).

5. Fill-up NTP Laboratory Request Form for DSSM (see Chapter IV, p. 56).Confirm three sputum collections.

TB Symptomatics are thosewith cough for 2 or more weekswith or without 1 or more of thefollowing:

• Fever• Chest and/or Back pains• Hemoptysis• Significant weight loss• Other symptoms, such as

sweating, fatigue, bodymalaise, shortness ofbreath

MICROSCOPY CENTER(To be accomplished by the medical technologist/microscopist)

1. Register in the NTP Laboratory Register (see chapter IV. p. 59)

2. Record date received and Laboratory Serial No. in the Laboratory Request Form forDSSM (see chapter IV. p. 56)

3. Perform DSSM: smearing, fixing, staining, and reading slides.

4. Record results in the Laboratory Request Form for DSSM (see chapter IV. p. 56) andin the NTPLaboratory Register (see chapter IV. p. 59)

5. Send back accomplished Laboratory Request Form for DSSM to the collection unit (see chapter IV. p. 56)

SPUTUM COLLECTION UNIT(To be accomplished by DOTS facility staff)

1. (Optional) Record results in the TB Symptomatics Masterlist (or TB SymptomaticsTarget Client List) (see Chapter IV, p. 54).

2. Explain result to the patient (If doubtful, immediately collect another 3 specimens forconfirmation).

3. Refer to physician/nurse.

DIAGNOSIS ANDINITIATION OF TREATMENT

6. Pack and send specimen/s to the Microscopy Center, together with thecompletely filled up NTP Laboratory Request Form for DSSM.

26

Figure 2.4. Guide to Diagnosis and Initiation of Treatment

CLINICAL DIAGNOSIS

To determine patient type and classification; done by DOTS facility staff

1. Verify information gathered on case finding.• Symptoms/condition of patient• Results of sputum examinations• Results of further examination (i.e., CXR, TBDC’s recommendations, culture, etc.)• Source of infection

2. Verify DSSM results.

3. Review history of previous treatment.• When was previous treatment taken? For how long?• Where was the previous treatment taken?• What anti-TB drugs were taken?• What was the DSSM result?• What was the treatment outcome?

To be done by INITIATION OF TREATMENT

Physician 1. Physical assessment and prescription of appropriatecategory of treatment regimen for TB patient according topatient classification and type

Nurse 2. Registration• Fill up NTP Treatment Card (see Chapter IV, p. 60).• Fill up two NTP ID Cards (see Chapter IV, p. 63), one

for treatment partner and one for patient.• Register in the TB Register (see Chapter IV, p. 65).

Designated DOTS Facility Staff 3. Health education with emphasis on key messages,such as:• TB is infectious.• TB can be cured but cure requires regular drug intake.• Irregular drug intake impedes cure and results in chronic

cases.• Anti-TB drugs have side-effects.• It is important to have follow-up DSSM examinations.• Family/treatment partner support is important.

Nurse 4. Intake of first dose• Record date when treatment started.• Record due date of the first DSSM follow-up in the

NTP Treatment Card (see Chapter IV, p. 60) andNTP ID Cards (see Chapter IV, p. 63).

Designated DOTS Facility Staff/Treatment Partners

5. DOT• Assign a treatment partner.• Do DOT for both intensive and continuation phases of

treatment.• Conduct weekly consultation meetings at the

DOTS facility during the whole course of treatment.

6. Record keeping• Maintain and update TB Register.• Maintain and update NTP Treatment Card at the DOTS facility.• See to it that both treatment partner and patient maintain, update, and keep NTP ID Cards.

Nurse/Midwife

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V. QUALITY ASSURANCE FOR DSSM

The quality assurance (QA) program is a series of regular activities carried out to monitor

the laboratory’s overall performance towards maintaining high quality results. DSSM results are

highly significant not only to the patient but also to the entire NTP. As such, it is essential for the

QA program to: 1) ensure that the reported results are accurate; 2) identify practices that are

potential sources of error; and 3) ensure that appropriate corrective actions are initiated.

A. OBJECTIVE

27

Assurance of high quality DSSM services in NTP

B. COMPONENTS

QA for DSSM includes the following:

1. Quality Control (QC) is the systematic internal monitoring of working practices, technical

procedure, equipment, and materials, including quality of stains. These are performed

regularly by the NTP medical technologist or microscopist.

2. External Quality Assessment (EQA) is a system of periodic independent measurement

of performance through collaboration with another competent laboratory at a higher level

(province or city). The trained NTP provincial or city coordinators and controllers are

responsible for EQA.

3. Quality Improvement (QI) is a process by which the components of smear microscopy

diagnostic services are analyzed by trained NTP provincial or city coordinators. This is

a continuous undertaking designed to identify and address problem areas, which in turn

will help ensure quality of DSSM services.

C. POLICIES

1. In the DOTS facility, the NTP-trained medical technologist/microscopist shall maintain

QC of routine work.

2. A Quality Assurance Center shall be established in every province and highly urbanized

city to ensure that QA activities are maintained in all DOTS facilities. Provincial/city health

offices are responsible for EQA, which includes blinded slide rechecking and on-site

evaluations by persons identified to perform such activities.

3. CHDs and their regional laboratories shall support the provincial/city QA centers.

Procedures and forms are found in the Manual on the Quality Assurance for Sputum Smear

Microscopy, March 2004.

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Case Holding

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Case holding is the procedure which ensures that patients complete their treatment. Chemotherapy

is currently the only way to stop the transmission of TB. While effective anti-TB drugs are available in

the country, there are still many TB patients who are not cured. This is because many patients stop

taking anti-TB drugs or they take their drugs irregularly. Patients are usually remiss in drug intake due

to the long duration of treatment. The shortest duration of treatment is six months.

Treatment compliance is necessary to cure TB and avoid development of drug resistance. It

is useless to search for cases if they could not be treated properly after they have been found. It would

only encourage false hopes on the part of the patient.

Poor treatment compliance may lead to the following outcomes: chronic infectious illness; drug

resistance; or death. Second-line anti-TB drugs for drug resistant cases are very expensive and most

are not available in the country. The best way to prevent the occurrence of drug resistance is through

regular intake of drugs for the prescribed duration. The strategy developed to ensure treatment

compliance is called Directly Observed Treatment (DOT). It is one of the key components of DOTS

towards achieving sufficient cure rate and preventing drug-resistant TB. DOT works by assigning a

responsible person to observe or watch the patient take the correct medications daily during the whole

course of treatment.

I. OBJECTIVE

Effective and complete treatment of TB cases, especially pulmonary sputum smear-positive cases

II. DEFINITION of TERMS

A. Classification of TB cases - TB cases shall be classified based on the location of lesions,

as well as the result of DSSM (Table 3.1).

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B. Types of TB cases - TB cases shall be categorized based on the history of anti-TB treatment(Table 3.2). A thorough understanding of the types of TB cases is necessary in determining thecorrect category of treatment regimen.

Table 3.1 Classification of TB Cases

Location of Lesion Definition of TermsDSSM Result

Pulmonary TB

(PTB)

Smear-Positive

1. A patient with at least two sputumspecimens positive for AFB, with or withoutradiographic abnormalities consistent withactive TB

OR2. A patient with one sputum specimen

positive for AFB and with radiographicabnormalities consistent with activepulmonary TB as determined by aphysician

OR3. A patient with one sputum specimen

positive for AFB and sputum culturepositive for M. tuberculosis

Smear-Negative

A patient with at least three sputum specimensnegative for AFB with radiographic abnormalitiesconsistent with active TB, and there has beenno response to a course of antibiotics and/orsymptomatic medications, and there is a decisionby a physician and /or TBDC to treat the patientwith a full course of anti-TB chemotherapy

Extra-PulmonaryTB (EP)

1. A patient with at least one mycobacterial smear/culture positivefrom an extra-pulmonary site (organs other than the lungs: pleura,lymph nodes, genito-urinary tract, skin, joints and bones, meninges,intestines, peritoneum, and pericardium, among others)OR

2. A patient with histological and/or clinical evidence consistent withactive extra pulmonary TB and there is a decision by a physicianto treat the patient with anti-TB drugs

Note: All EP cases shall undergo DSSM prior to treatment.

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Table 3.2. Types of TB Cases

Note: *Treatment for primary and latent tuberculosis infection should not be considered as a previous TB treatment.

C. Directly Observed Treatment (DOT) - DOT is a method developed to ensure treatment compliance

by providing constant and motivational supervision to TB patients. DOT works by having a responsible

person, referred to as treatment partner, watch the TB patient take medicines everyday during

the whole course of treatment.

Any of the following could serve as treatment partner: a) DOTS facility staff, such as the

midwife or the nurse; or b) a trained community member, such as the BHW, local government

official, or former TB patient. A member of the patient’s family may not be as reliable as a health

worker in serving as treatment partner, but he/she may be assigned as treatment partner

during weekends and holidays.

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Types of TB Cases Definition of Terms

New A patient who has never had treatment for TB or who has taken anti-TB drugs for less than one month

Relapse A patient previously treated for TB, who has been declared cured ortreatment completed, and is diagnosed with bacteriologically positive(smear or culture) TB

Treatment Failure A patient who, while on treatment, is sputum smear-positive at fivemonths or later during the course of treatment

Return AfterDefault(RAD)

A patient who returns to treatment with positive bacteriology (smear orculture), following interruption of treatment for two months or more

Transfer-in A patient who has been transferred from another facility adopting NTPpolicies with proper referral slip to continue treatment

Other All cases who do not fit into any of the above definitions.

This may also include the following:1. Other (positive) – a patient who was initially registered as a new

smear-negative case and turned out to be smear-positive duringtreatment;

2. Other (negative) – a patient who interrupted treatment for two ormore months and has remained or become smear-negative uponreturn for treatment; and

3. Chronic case – a patient who remains sputum-positive at the endof a re-treatment regimen.

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DOT can be done in any accessible and convenient place for the patient (e.g., DOTS

facility, treatment partner’s house, patient’s place of work, or patient’s house) as long as the

treatment partner can effectively ensure the patient’s intake of the prescribed drugs and monitor

his/her reactions to the drugs. It is important to supervise the smear-positive TB patients’ daily

anti-TB drug intake during the intensive and continuation phases of short-course chemotherapy.

III. POLICIES

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diagnostic technique, namely, DSSM.

b. Domiciliary treatment shall be the preferred mode of care.

c. Patients with the following conditions shall be recommended for hospitalization:

1. massive hemoptysis;

2. pleural effusion obliterating more than one-half of a lung field;

3. miliary TB;

4. TB meningitis;

5. TB pneumonia; and

6. those requiring surgical intervention or with complications.

d. All patients undergoing treatment shall be supervised (DOT). No patient shall initiate

treatment unless the patient and DOTS facility staff have agreed upon a case holding

mechanism for treatment compliance.

e. The national and local government units shall ensure provision of drugs to all smear-

positive TB cases.

There are two formulations of anti-TB drugs:

1. Fixed–dose combination (FDCs) – Two or more first-line anti-TB drugs are combined

in one tablet. There are 2-, 3-, or 4-drug fixed-dose combinations.

2. Single drug formulation (SDF) – Each drug is prepared individually: INH, ethambutol,

and pyrazinamide are in tablet form while rifampicin is in capsule form. These

drugs are usually in blister packs good for one week.

The Department of Health shall ensure the provision of FDC drugs to LGUs and other

DOTS facilities for all TB cases, giving priority to smear-positive cases. However, LGUs shall

procure a portion (at least 5% of the expected cases) of the requirements for SDF for those with

adverse reactions necessitating withdrawal of FDC and for Category III cases.

f. Quality of FDCs must be ensured. FDCs must be ordered from a source with a track record

of producing FDCs according to WHO-prescribed strength and standard of quality.

g. Treatment shall be based on recommended category of treatment regimen (Table 3.3).

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Table 3.3. Recommended Category of Treatment Regimen

h. Dosage per Category of Treatment Regimen

a. Fixed-Dose Formulation

The number of tablets of FDCs per patient will depend on the body weight. Hence, all patients

must be weighed (using kilogram as a unit) before treatment is started. Tables 3.4 and 3.5 show the

treatment regimens for specific categories while Annex 2 shows sample packages of FDCs and SDFs.

I New smear-positive PTB,New smear-negative PTB withextensive parenchymallesions on CXR as assessedby the TBDC, EPTB, andsevere concomitant HIVdisease

2HRZE 4HR

II Treatment Failure, Relapse,RAD, Other

2HRZES/HRZE 5HRE

III New smear-negative PTB withminimal parenchymal lesionson CXR as assessed by theTBDC

2HRZE 4HR

IV Chronic (still smear-positiveafter supervised re-treatment)

Refer to specialized facility orDOTS Plus Center

Refer to Provincial/City NTPCoordinator

Category Type of TB PatientTB Treatment Regimens

Intensive Phase Continuation Phase

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Table 3.4. Treatment Regimen for Categories I & III: 2HRZE/4HR (FDC)

Table 3.6. Treatment Regimen for Categories I & III: 2HRZE/4HR (SDF)

Table 3.5. Treatment Regimen for Categories II: 2HRZES/HRZE/5HRE (FDC)

0.75 g

0.75 g

0.75 g

0.75 g

b. Single Drug Formulation

Simply add one tablet of INH (100mg), PZA (500mg), and E (400mg) each for the patient weighing

more than 50kg before treatment initiation. Modify drug dosage within acceptable limits according to

patient’s body weight, particularly those weighing less than 30kg at the time of diagnosis (Table 3.8).

Body Weight (kg) Intensive Phase Continuation Phase

30-37

38-54

55-70

> 70

First Two months Third month

FDC-A(HRZE)

STREPTOMYCINFDC-A(HRZE)

FDC-B(HR)

E400 mg

2

3

4

5

2

3

4

5

2

3

4

5

1

2

3

3

ANTI-TB Drugs No. of Tablets per DayIntensive Phase

(2 months)

No. of Tablets per DayContinuation Phase

(4 months)

Isoniazid (H) 300mg

Rifampicin (R) 450mg

Pyrazinamide (Z) 500mg

Ethambutol (E) 400mg

1

1

2

2

1

1

Body Weight (kg) No. of Tablets per DayIntensive Phase

(2 months)FDC-A (HRZE)

No. of Tablets per DayContinuation Phase

(4 months)FDC-B (HR)

30-37

38-54

55-70

> 70

2

3

4

5

2

3

4

5

750 mg

750 mg

750 mg

750 mg

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Table 3.7. Treatment Regimen for Categories II: 2HRZES/HRZE/5HRE (SDF)

* 56 vials for two months

Table 3.8. Drug Dosage per KG Body Weight

Drug Dose per kg body weight and maximum dose

Isoniazid

Rifampicin

Pyrazinamide

Ethambutol

Streptomycin

5 (4-6) mg/kg, and not to exceed 400mg daily

10 (8-12) mg/kg, and not exceed 600mg daily

25 (20-30) mg/kg, and not to exceed 2g daily

15 (15-20) mg/kg, and not to exceed 1.2g daily

15 (12-18) mg/kg, and not to exceed 1g daily

ANTI-TB Drugs No. of tablets per dayIntensive Phase

(3 months)

No. of tablets per dayContinuation Phase

(5 months)

Isoniazid (H) 300mg

Rifampicin (R) 450mg

Pyrazinamide (Z) 500mg

Ethambutol (E) 400mg

Streptomycin (S) 1gm

First 2 months

1

1

2

2

1 vial/day*

3rd month

1

1

2

2

1

1

2

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IV. PROCEDURES

A. Initiation of Treatment and Registration

1. Inform the patient that he/she has TB and motivate him/her to undergo treatment.

2. Refer patient living outside the catchment area to the most accessible DOTS

facility where his/her treatment can be supervised.

3. Weigh the patient.

4. Refer patient to a physician for pre-treatment evaluation.

5. Open the NTP Treatment Card and two NTP ID Cards (one for treatment partner

and one for patient) and start the treatment.

6. Watch patient swallow the initial dose.

7. Register patient in the TB Register.

B. Ensuring Treatment Compliance through DOT

1. Together with the patient, identify a treatment partner.

2. Explain the importance of treatment compliance to the patient.

3. Administer patient’s drugs daily. Emphasize the following to both patient and

treatment partner:

a. Patient and treatment partner should meet at their agreed treatment

unit everyday.

b. Drugs should be taken 2-3 hours after a regular meal.

c. Treatment partner should make sure that the patient swallows his/her

drugs daily.

d. After intake of drugs, treatment partner should sign the

treatment partner’s NTP ID Card, as well as the patient’s NTP ID Card.

4. Motivate treatment partner to be vigilant about patient’s treatment regimen.

a. On Saturdays, Sundays, and holidays, when the DOTS facility is closed,

Treatment could be done at home but should be supervised by a trained

family member.

b. Treatment partner should emphasize key messages, such as:

• TB can be cured but cure requires regular drug intake for the

prescribed duration.

• Patient should report any adverse drug reaction.

• Patient should undergo follow-up sputum examination on specified

dates. Schedule of DSSM follow-up for Categories I and III patients

is shown in Table 3.9 while Table 3.9.a shows the schedule for those

in Category II.

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1Check DSSM follow-up results at the end of treatment (during the last week of treatment) for the patient who was smear-positive in the last DSSM follow-up and smear-negative in the repeated DSSM (Tables 3.10, and 3.10.a, and Figures 3.1, and 3.3).

Table 3.9 Schedule of DSSM Follow-up (Categories I and III)

Schedule of

DSSM

Follow-up

Category I

(2HRZE/4HR)

Regular Treatment

With One-Month

Extension(HRZE)

Category III

(2HRZE/4HR)

Regular Treatment

Towards end of

2nd month

Towards end of

3rd month

Towards end of

4th month

Towards end of

5th month

Beginning of

6th month

Beginning of

7th month

YES

(If negative)

YES

YES1

(If positive)

YES

YES

YES1

YES

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Table 3.9.a Schedule of DSSM Follow-up (Category II)

1Check DSSM follow-up results at the end of treatment (during the last week of treatment) for patients who were smear-positive in the last DSSMfollow-up and smear-negative in the repeated DSSM (Tables 3.10.b, and 3.10.c, and Figures 3.2).

Schedule of

DSSM

Follow-up

Towards end of

2nd month

Towards end of

3rd month

Towards end of

4th month

Towards end of

5th month

Towards end of

6th month

Towards end of

7th month

YES

(If negative)

YES1

(If positive)

YES

YES1

Category II (2HRZES/HRZE/5HRE)

Regular Treatment With One-MonthExtension (HRZE)

Beginning of

8th month

Beginning of

9th month

YES

YES

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5. Conduct regular (preferably weekly) consultation meetings with patient and treatment partner

for treatment evaluation at the DOTS facility.

6. Exert effort to contact patient when he/she fails to report on due date.

C. Monitoring Response to Treatment

1. Monitor sputum smear status of all patients under treatment, including initially sputum-smear

negative patients, according to the standard schedule (Tables 3.9 and 3.9.a).

2. Modify treatment based on DSSM follow-up results (Tables 3.10, 3.10.a, 3.10.b, and 3.10.c,

and Figures 3.1, 3.2, and 3.3).

Treatment Modifications Based on Results of DSSM Follow-up

1. Do DSSM follow-up towards the end of the second month of treatment.

2. If the result is negative, start continuation phase (HR) and follow recommendations in Table

3.10.

3. If the result is positive, extend intensive phase (HRZE) for another month.

Refer to Table 3.10.a for treatment modifications of smear-positive patients after follow-up

examination.

Category I Treatment Regimen

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Table 3.10. Treatment Modification for New PTB Smear-Positive Cases Based on the Results of

DSSM Follow-up for Category I Treatment Regimen Without Extension

1Check DSSM follow-up results towards the end of the sixth month of treatment only for patients who are: 1) smear-positive in the beginning of the6

th month and smear-negative in the repeated DSSM; and 2) smear-positive towards the end of the fourth month but turned out to be negative in

the beginning of the 6th

month.

Towards end of

4th MonthBeginning of 6th Month Towards end of 6th

Month1

If smear-negative,

continue

continuation phase

(HR).

If smear-negative, complete continuationphase until end of treatment course anddeclare as cured.

If smear-positive,repeat DSSMimmediately forconfirmation andconsult DOTSPhysician

If smear-negative in therepeated DSSM,continue continuationphase (HR) and doDSSM towards end of6th month of treatment.

If smear-positive againin the repeated DSSM,declare as Failed; re-register as TreatmentFailure and start withCategory II treatmentregimen.

If smear-negative,declare as cured.

If smear-positive, declareas Failed; re-register asTreatment Failure and startwith Category II treatmentregimen.

If smear-positive,continue continuationphase (HR).

If smear-negative, continue continuation phase(HR) and do DSSM towards end of 6th monthof treatment.

If smear-negative,declare as cured.

If smear-positive, declareas Failed; re-register asTreatment Failure andstart with Category IItreatment regimen.

If smear-positive, declare as Failed, re-registeras Treatment Failure and start with CategoryII treatment regimen.

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Table 3.10.a Treatment Modification for New PTB Smear-Positive Cases Based on the Results

of DSSM Follow-up for Category I Treatment Regimen With Extension

1Check DSSM follow-up results towards the end of the seventh month of treatment only for patients who are: 1) smear-positive in the beginningof the seventh month and smear-negative in the repeated DSSM; and 2) smear-positive towards the end of the fifth month and turned out tobe negative in the beginning of the seventh month.

If smear-positive, declare asfailed; re-register as Treatmentfailure and start Category IItreatment regimen

TowardsEnd of 3rd

Month

Towards Endof 5th Month Beginning of 7th Month Towards End of 7th

Month1

If smear-negative, startcontinuationphase (HR).


If smear-positive,repeat DSSMimmediately forconfirmation andconsult DOTSphysician.

If smear-negative inthe repeatedexamination, continuecontinuation phase(HR) and do DSSMtowards end of 7th

month of treatment.

If smear-positive in therepeated examination,declare as failed; re-register as treatmentfailure and startCategory II treatmentregimen.

If smear-negative, declare ascured

If smear-negative,continuecontinuationphase (HR).

If smear-positive,continuecontinuationphase (HR).

If smear-negative, declare ascured.

If smear-positive, declare as failed;re-register as treatment failureand start Category II treatmentregimen.

If still smear-positive, declare as failed;re-register as treatment failure and startCategory II treatment regimen.

If smear-negative, continue continuationphase (HR) and do DSSM towards end of 7th month of treatment.

If smear-positive, startcontinuationphase (HR).

If smear-negative, continuecontinuationphase (HR).



If smear-negative inthe repeatedexamination, continuecontinuation phase(HR) and do DSSMtowards end of 7th

month of treatment.

If smear-negative, declare ascured.

If smear-positive, declare asfailed; re-register as treatmentfailure and start Category IItreatment regimen

If smear-positive in therepeated examination,declare as failed; re-register as treatmentfailure and start CategoryII treatment regimen.

If still smear-positive, declare asfailed; re-register astreatment failure andstart Category IItreatment regimen.

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Table 3.10.b Treatment Modification for PTB Smear-Positive Cases Based on the Results of

DSSM Follow-up for Category II Treatment Regimen Without Extension

1. Do DSSM follow-up towards the end of the third month of treatment.

2. If DSSM result is negative, start continuation phase (HRE) and refer to Table 3.10.b.

3. If DSSM result is positive, extend intensive phase (HRZE) treatment for another month. Refer

to Table 3.10.c.

Category II Treatment Regimen

1Check DSSM follow-up results towards the end of the 8

thmonth of treatment only for patients who are: 1) smear-positive in the beginning of the 8

th

month and smear-negative in the repeated DSSM; 2) smear-positive towards the end of the 5th

month and turned out to be negative in the beginningof the 8

th month.

Towards End of5th Month

Beginning of 8th Month Towards End of 8th

Month1

If smear- negative,continue continuationphase (HRE).

If smear-negative, complete continuation phaseuntil the end of the treatment course and declareas cured.


If smear-negative in therepeated DSSM,continue continuationphase (HRE) and doDSSM towards end of8th month.

If smear-negative,declare as cured

If smear-positive,declare as failed

If smear- positive,continue continuationphase (HRE).

If smear-negative, continue continuation phase(HRE) and do DSSM towards end of 8th month.

If smear-negative,declare as cured

If smear-positive,declare as failed.

If smear-positive, complete continuation phase(HRE) until end of treatment course and declareas failed.

If smear-positive again inthe repeated DSSM,complete continuationphase (HRE) until end oftreatment course anddeclare as failed.

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1Check DSSM follow-up results towards the end of the ninth month of treatment only for patients who are: 1) smear-positive in the beginning ofthe ninth month and smear-negative in the repeated DSSM; and 2) smear-positive towards the end of the sixth month and turned out to be negativein the beginning of the ninth month.

Table 3.10.c Treatment Modifications for PTB Smear-Positive Cases Based on DSSM Follow-up

for Category II Treatment Regimen With Extension

Towards Endof 4th Month

Towards Endof 6th Month

Beginning of 9th Month Towards End of9th Month1

If smear-positive orsmear-negative, startcontinuationphase (HRE).

If smear-negative,continuecontinuationphase (HRE).

If smear-negative, completecontinuation phase until end oftreatment course and declare as cured

If smear-positive, repeatDSSMimmediately forconfirmationand consultDOTSphysician.

If smear-negative inthe repeated DSSM,continuecontinuation phase(HRE) and doDSSM towards endof 9th month oftreatment.

If smear- negative,declare as cured.

If smear- positive,declare as failed.

If smear positiveagain in therepeated DSSM,completecontinuation phase(HRE) until end oftreatment anddeclare as failed.

If smear- positive,continuecontinuationphase (HRE).

If smear negative, continuecontinuation phase (HRE) and doDSSM towards end of 9th month oftreatment.

If smear- negative,declare as cured.

If smear-positive,completecontinuation phase(HRE) until end oftreatment courseand declare asfailed.

If still smear-positive, completecontinuation phase (HRE) until end oftreatment and declare as failed.

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*Check DSSM follow-up results at the end of treatment for patients who were smear-positive in the last DSSM follow-up and smear-negative in therepeated DSSM.

H R Z ES H R E

1st mo. 2nd mo. 3rd mo. 4th mo. 5th mo. 6th mo. 7th mo. 8th mo. 9th mo.

*

1. Do DSSM follow-up towards the end of 2nd month of treatment.

2. If the result is negative, start continuation phase (HR).

3. If the result is positive, declare as Failed, re-register as Other, and start Category II treatment

regimen.

Category III Treatment Regimen

Summary of Treatment Modification Based on DSSM Follow-up Results

Figure 3.1. Category I Treatment Modification Based on DSSM Follow-up Results*

*

1st mo. 2nd mo. 3rd mo. 4th mo. 5th mo. 6th mo. 7th mo.

H R Z E H R

*

CATEGORY - I

Figure 3.2. Category II Treatment Modification Based on DSSM Follow-up Results*CATEGORY - II

Figure 3.3. Category III Treatment Modification Based on DSSM Follow-up Results*

CATEGORY – III

1st mo. 2nd mo. 3rd mo. 4th mo. 5th mo. 6th mo.

H R Z E H R

H R Z E

If positive,

H R

If negative,

H R Z EWith Extension

If positive,H R E

If negative,

H R Z EWith Extension

*

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Table 3.11. Guide in Managing Adverse Reactions to Anti-TB Drugs

D. Management of Adverse Reactions to Drugs

Closely monitor the occurrence of minor and major reactions to drugs, especially during

the intensive phase. (Table 3.11). There are major side effects that necessitate withdrawal of the

responsible drug. Since FDC drugs are already used, there is a need to switch to SDF whenever

side effects to one or more components of the FDC are suspected.

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For details on the management of adverse drug reactions, refer to the Interventions for Tuberculosis Control

and Elimination [International Union Against Tuberculosis and Lung Disease (2002), pp. 87-91].

2. Jaundice due to hepatitis Any kind of drugs(especially Isoniazid,Rifampicin, andPyrazinamide)

Discontinue anti-TB and refer to DOTSphysician

If symptoms subside, resume treatment andmonitor clinically.

3. Impairment of visual acuityand color vision due to opticneuritis

Ethambutol Discontinue Ethmbutol and refer to anophthalmologist.

4. Hearing impairment, ringingof the ear, and dizziness dueto damage of the eihthcranial nerve

Streptomycin Discontinue Streptomycin and refer to DOTSphysician.

5. Oliguria or albuminuriadue to renal disorder

StreptomycinRifampicin

Discontinue anti-TB drugs and refer to DOTSphysician.

6. Psychosis and convulsion Isoniazid Discontinue Isoniazid refer to DOTS physician.

7. Thrombocytopenia, anemia,shock

Rifampicin Discontinue anti-TB drugs and refer to DOTSphysician.

Give anti-histamines.

Reassure the patient

Minor

1. Gastro-intestinal intolerance Rifampicin/INH Give medication at bedtime or give small meals.

2. Mild skin reactions Any kind of drugs

3. Orange/red colored urine Rifampicin

4. Pain at the injection site Streptomycin Apply warm compress. Rotate sites of injection.

5. Burning sensation in the feetdue to peripheral neuropathy

Isoniazid Give Pyridoxine (Vitamin B6):100-200mg dailly for treatment10mg daily for prevention.

6. Arthralgia due tohyperuricemia

Pyrazinamide Give aspirin or NSAID.

If symptoms persist, consider gout and requestfor blood chemistry (uric acid determinationand manage accordingly).

7. Flu-like symptoms (fever,muscle pains, inflammationof the respiratory tract)

Rifampicin Give antipyretics.

Major

1. Severe skin rash due tohypersensitivity

Any kind of drugs(especially Streptomycin)

Discontinue anti-TB drugs and refer to DOTSphysician.

Adverse Reactions Drug(s) probablyresponsible Management

45

E. Management of Cases Who Interrupted Treatment

1. Perform routine DSSM on defaulters who come back for chemotherapy. Refer patients to

DOTS physician for re-evaluation and re-treatment.

2. Manage new smear-positive patients who interrupted treatment according to recommended

treatment modification (Table 3.12).

3. Manage Relapse and Treatment failure cases who interrupted treatment according to recommended

treatment modification (Table 3.12.a).

4. Continue treatment for patients who were referred or transferred with proper referral slip.

However, do DSSM on patients without properly accomplished referral slip.

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Table 3.12 Treatment Modifications for New Smear-Positive Cases Who Interrupted Treatment

1This is the exceptional case categorizing as Defaulted a patient who interrupted treatment at less than 8 weeks.

Length oftreatment

Less than onemonth

Length ofInterruption

Do asmear?

Result ofsmear

Register again? Treatmentmodification

Less than 2weeks

No No, use same treatmentcard.

Continue Category ITreatment Regimen

2 weeks or more Yes No, open a new treatmentcard (Use same TB casenumber).

Restart Category ITreatment Regimenagain

Positive

No, use same treatmentcard.


Negative

One to twomonths

Less than 2weeks



2 to 8 weeks

Yes


Complete remainingintensive phase; addone extra month ofintensive phase.

Positive


Continue Category ITreatment Regimen.

Negative

Yes

Close previous registrationas Defaulted; re-register asRAD and open a newtreatment card (new TBcase number).

Start Category IITreatment Regimen

Positive

Close previous registrationas Defaulted; re-registerunder Other and open anew treatment card. (NewTB case number).


Negative

More than 8weeks but stillwithin 6-monthtreatmentregimen

More than twomonths

Less than 2weeks



2 to 8 weeks

Yes

Close previous registrationas Defaulted1; re-registeras RAD and open a newtreatment card. (New TBcase number).

Start

Category II TreatmentRegimen

Positive


Continue Category ITreatment Regimen.

Negative

Yes

Close previous registrationas Defaulted; re-register asRAD and open a newtreatment card. (New TBcase number).


Positive

Close previous registrationas Defaulted; re-registerunder Other and open anew treatment card (NewTB case number).


Negative


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Table 3.12.a Treatment Modifications for Relapse and Treatment Failure Cases Who Interrupted

Treatment

1This is the exceptional case categorizing as Defaulted a patient who interrupted treatment at less than 8 weeks.

Length oftreatment

Less than onemonth

Length ofInterruption

Do aDSSM?

Result ofDSSM

Register again? Treatmentmodification

Less than 2weeks


Continue Category IITreatment Regimen

2 weeks or more Yes No, open a new treatmentcard.

Restart Category IITreatment Regimen

Positive



Negative

One to twomonths

Less than 2weeks



2 to 8 weeks

Yes


Complete remainingintensive phase; addone extra month ofintensive phase.

Positive


Continue Category IITreatment Regimen.

Negative

Yes

Close previous registrationas Defaulted; re-register asRAD and open a newtreatment card.


Positive

Close previous registrationas Defaulted; re-registerunder Other and open anew treatment card.


Negative


More than twomonths

Less than 2weeks



2 to 8 weeks

Yes

Close previous registrationas Defaulted1; re-registeras RAD and open a newtreatment card.


Positive


Continue Category IITreatment Regimen.

Negative

Yes

Close previous registrationas Defaulted; re-register asRAD and open a newtreatment card.


Positive

Close previous registrationas Defaulted; re-registerunder Other and open anew treatment card.


Negative


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F. Management of Referred Cases

1. Assess and categorize all TB cases properly referred for continuation of treatment by other

DOTS facilities as Trans-in and manage them in accordance with NTP policies and guidelines.

Return the duplicate referral form to the referring unit.

2. Evaluate all other referred patients in accordance with NTP policies and guidelines.

G. Management of TB in Special Situations*

1. Pregnancy

Ascertain whether or not a woman is pregnant before she starts TB treatment. Most

anti-tuberculosis drugs are safe for pregnant women, except Streptomycin, which is ototoxic

to the fetus. Advise a pregnant woman that successful treatment of TB with the recommended

standardized treatment regimen is important for a successful outcome of pregnancy.

2. Breastfeeding

A breastfeeding woman afflicted with TB should receive a full course of TB treatment.

Timely and properly applied chemotherapy is the best way to prevent transmission of tubercle

bacilli to the baby. All anti-tuberculosis drugs are compatible with breastfeeding. A woman

taking these drugs can safely continue to breastfeed. Mother and baby should stay together

and the baby may be breastfed in the normal way. Give the baby prophylactic isoniazid for at

least three months beyond the time the mother is considered to be non-infectious. Defer BCG

vaccination of the newborn until the end of isoniazid prophylaxis.

3. Oral Contraceptives

Rifampicin interacts with oral contraceptive medications with a risk of decreased

protective efficacy against pregnancy. Advise a woman receiving oral contraceptives while on

rifampicin treatment that she has the following options: 1) take an oral contraceptive pill

containing a higher dose of estrogen (50 ), following consultation with a clinician; or 2) use

another form of contraception.

4. Liver Disorders

Isoniazid, rifampicin, and pyrazinamide are all associated with hepatitis. Of the three

drugs, rifampicin is least likely to cause hepatocellular damage, although it is associated with

cholestatic jaundice. Of the three agents, pyrazinamide is the most hepatotoxic.

Patients with the following conditions can receive the usual short course chemotherapy

regimens provided there is no clinical evidence of chronic liver disease: hepatitis virus carriage;

a past history of acute hepatitis; and excessive alcohol consumption. However, hepatotoxic

reactions to antituberculosis drugs may be more common among these patients and should

therefore be anticipated.

* Source: Treatment of Tuberculosis: Guidelines for National Programs WHO/CDS/TB 2003.313

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5. Established Chronic Liver Disease

Patients with liver disease should not receive pyrazinamide. Isoniazid plus rifampicin

plus one or two non-hepatotoxic drugs, such as streptomycin and ethambutol, can be used

for a total duration of eight months. Alternative regimens are 9RE or 9SHE in the intensive

phase, followed by HE in the continuation phase, with a total treatment duration of 12 months.

Recommended treatment regimens are therefore 2SHRE/6HR, 9RE, or 2SHE/10HE.

6. Acute Hepatitis (e.g., Acute Viral Hepatitis)

It is not common for a patient to have TB concurrently with acute hepatitis unrelated

to TB or TB treatment. Clinical judgment is necessary. In some cases, it is possible to defer

TB treatment until the acute hepatitis has been resolved. In other cases, when it is necessary

to treat TB during acute hepatitis, the combination of SE for three months is the safest option.

If the hepatitis has been resolved, then put the patient on a continuation phase of six months

isoniazid and rifampicin (6HR). If the hepatitis has not been resolved, SE should be continued

for a total of 12 months.

7. Renal Failure

Isoniazid, rifampicin, and pyrazinamide are either eliminated almost entirely by

biliary excretion or metabolized into non-toxic compounds. These drugs, therefore, can be

given in normal dosages to patients with renal failure. Patients with severe renal failure

should receive isoniazid with pyridoxine to prevent peripheral neuropathy.

Streptomycin and ethambutol are excreted by the kidney. Where facilities are

available to monitor renal function closely, streptomycin and ethambutol may be given in

reduced doses. The safest treatment regimen for patients with renal failure is 2HRZ/4HR.

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8. Treating TB and HIV*

In patients with HIV-related TB, the priority is to treat TB, especially smear-positive

PTB to stop transmission. However, patients with HIV-related TB can have Anti-Retroviral

Therapy (ART) and anti-TB treatment at the same time, if managed carefully. Careful

evaluation is necessary in judging when to start ART. In the case, for example, of a patient

with a high risk of death during the period of TB treatment (i.e. disseminated TB and/or CD4

count <200/mm3), it may be necessary to start ART concomitantly with TB treatment. On

the other hand, for a patient with smear-positive PTB as the first manifestation of HIV

infection, who does not appear to be at risk of dying, it may be safer to defer ART until the

initial phase of TB treatment has been completed. This decreases the risk of immune

reconstitution syndrome and avoids the risk of drug interaction between Rifampicin and a

Protease Inhibitor (PI).

Possible options for ART in patients with TB includes the following:

* Source: TB/HIV A Clinical Manual, 2nd Edition WHO/HTM/TB/2004.329

• Defer ART until completion of TB treatment.

• Treat TB with a Rifampicin-containing regimen and use efavirenz + two Nucleoside

Reverse Transcriptase Inhibitors (NsRTIs).

• Defer ART until the completion of the initial phase of TB treatment and then use

Ethambutol and Isoniazid in the continuation phase.

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V. Treatment Outcome

A. Cured - a sputum smear-positive patient who has completed treatment and is sputum smear-

negative in the last month of treatment and on at least one previous occasion in the continuation

phase

B. Completed Treatment - a patient who has completed treatment but has not met the criteria

for cure or failure

This group includes:

• A sputum smear-positive patient who has completed treatment but without DSSM follow -

up during the treatment, or with only one negative DSSM during the treatment, or without

DSSM in the last month of treatment.

• A sputum smear-negative patient who has completed treatment

C. Died - a patient who died for any reason during the course of treatment

D. Failed

• A patient who is sputum smear-positive at five months or later during the treatment

• An initially sputum smear-negative patient before starting treatment who becomes

smear-positive during the treatment. (Note: This case will be re-registered as Other with

a new TB case number.)

E. Defaulted - a patient who interrupted treatment for two consecutive months or more

F. Transferred out: A patient who transferred to another DOTS facility with proper referral slip

for continuation of treatment and whose treatment outcome is not known

VI. Summary Guides

The case holding procedure is summarized in the following Guide to Case Holding

and the accompanying Guide to Ensuring Treatment.

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Figure 3.4. Guide to Caseholding

AT THE TREATMENT UNIT (DOTS Facility)

To be done by DOTSfacility staff

1. Conduct health education for both patient and his/her family. Emphasize thefollowing key messages:• Importance of regular drug intake;• Results of irregular drug intake;• Side effects of anti-TB drugs;• Necessity of DSSM follow-up; and• Importance of family and treatment partner support.

2. Conduct regular consultation meetings with patient and treatment partnerduring the course of treatment.

To be accomplishedby DOTS facility staffand treatment partner

3. Monitor and record treatment regularity.• TB Register (nurse) (see Chapter 4, p. 67)• NTP Treatment Card (midwife) (see Chapter 4, p. 60)• NTP ID Card (Treatment Partner and TB patient) (see

Chapter 4, p. 63)

To be accomplished byDOTS facility staff

4. Do DSSM follow-up on time.• Label container with the name of the patient.• Collect 1 sputum specimen (preferably early morning specimen).• Fill up the NTP Laboratory Request Form for DSSM (see Chapter 4, p. 56).Pack

the specimens securely and send to microscopy center, together with dulyaccomplished NTP Laboratory Request Form for DSSM

AT THE MICROSCOPY CENTER(To be accomplished by the Medical Technologist or Microscopist)

Register in the NTP Laboratory Register (see Chapter 4, p. 59).

Smear, fix, stain, and do microscopic examination.

Record the results in the NTP Laboratory Request Form for DSSM.

(see Chapter 4, p. 57) and in the NTP Laboratory Register (see Chapter 4, p. 59)

Send the NTP Laboratory Request Form for DSSM to the treatment unit.

AT THE TREATMENT UNIT (DOTS Facility)

To be accomplishedby DOTS facility staff

Record DSSM results and due date of DSSM follow-up examination in the NTPTreatment Card ((see Chapter 4, p. 60). Any follow-up examination with smear-positive results must be referred to the physician.


Record the results in the TB Register. (see Chapter 4, p. 67).


Inform treatment partner of DSSM results so that he/she can update the NTP IDCard (see Chapter 4, p. 63).


Upon Treatment Completion:1. Evaluate and record treatment outcome in the TB Register (see Chapter 4,

p. 67) and NTP Treatment Card (see Chapter 4, p. 60).2. Prepare and submit the Quarterly Report on Treatment Outcome (see Chapter

4, p. 79).

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Figure 3.5 Guide to Ensuring Treatment

Recorded information should be checked to ensure consistency of records of TB patients

(To be accomplished by DOTS facility staff)Record of Individual patients

• TB Case number

• Classification, type, and regimen

• DSSM results on diagnosis, for follow-up

• Drug collection

• Defaulter action

• Treatment outcome

NTP Treatment Card

(To be accomplished by the MT)Record of laboratory examinationresults

- 3 sputum collections- DSSM results on diagnosis / for

follow-up

NTP Laboratory RegisterThe nurse should check the followinginformation weekly:- is diagnosis correct?- is treatment regimen approriate?- are all smear-positive cases registered and

treated properly with DOT?- are drugs collected on time?- are follow-up exams done on time?- are treatments regular and effective?- are actions taken to retrieve defaulters?

(To be accomplished by the DOTS facility staff)Record of Treatment Activity in the DOTS Facility

• TB Case number

• Classification, type, and regimen

• DSSM results on diagnosis, and for follow-up

• Defaulter action

• Treatment outcome

TB Register

Recording and Reporting

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Recording and reporting are important in the implementation of a successful TB control program.

Availability of records ensures provision of appropriate and effective care for patients. Through efficient

recording, health workers can monitor that each TB symptomatic found is examined and cured. Records,

therefore, should contain accurate, complete, and up-to-date information on patient’s diagnosis,

treatment, follow-up examinations, and treatment outcome.

Aside from information on patient’s coverage and care, records also provide information on

program efficiency and effectiveness, as well as availability of drugs and other NTP supplies at the

DOTS facilities. This section of the Manual of Procedures is designed to generate and provide the

minimum set of information, through various forms, required for program planning at different levels.

I. OBJECTIVES

1. Provision of information that would help program implementers plan on how best to improve

the quality of DOTS services.

2. Provision of information that would help program supervisors plan on how best to assist TB

control program implementers

II. POLICIES

1. Recording and reporting for NTP shall be implemented at all DOTS facilities in the country,

including Public-Private Mix DOTS units, and government and private hospitals.

2. Recording and reporting shall include all cases of TB, classified according to internationally

accepted case definitions.

3. Recording and reporting for NTP shall use the FHSIS network for routine reporting and feedback.

4. Records and reports shall allow for the calculation of the main indicators for program evaluation

(see Chapter VI Monitoring, Supervision and Evaluation).

5. All quarterly reports should be sent to the DOH through channels (DOTS facility to PHO/CHO

to CHD to NCDPC-DOH). Quarterly reports should reflect the additionality of cases reported

from various units in the province/city/municipality (e.g. PPMD, hospitals, NGOs).

III. NTP RECORDING FORMS

These are the recording forms used by the NTP:

• TB Symptomatics Masterlist/TB Symptomatics Target Client List (Optional);

• NTP Laboratory Request Form for DSSM;

• NTP Laboratory Register;

• NTP Treatment Card;

• NTP Identification Card;

• TB Register;

• TBDC Masterlist;

• NTP Referral Form; and

• TBDC Referral Form

For recording forms used in the Quality Assurance for sputum microscopy, please refer to the

Manual on Quality Assurance for Sputum Microscopy.

1. TB Symptomatics Masterlist /TB Symptomatics Target Client List

(Optional)

This record confirms the three sputum collections done at the DOTS facilities. Maintained

by the designated DOTS facility staff, the TB Symptomatics Target Client List of FHSIS may

be used in areas where the TB Symptomatics Masterlist is not available.

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TB SYMPTOMATICS MASTERLIST

FamilySerialNo.(1)

Date ofRegis-tration

(2)

Name(3)

Address(4)

Age(5)

Sex(5)

Date SputumCollected/Examiation

Results

X-RayExamination

TBCase

Number(11)

Remarks(12)

1st

(7) 2nd

(8)Date

referredfor X-ray

(9)

Date &Result (10)

Following are the information needed for each item on the TB Symptomatics Masterlist (to be filled

out by the midwife or any designated DOTS facility staff):

(1) Family serial number based on the family consultation record or annual serial number for

TB symptomatics in the clinic

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(5) Patient’s age in years

(6) Patient’s sex (M for male and F for female)

(7) Date (mm/dd/yy) when each sputum specimen was collected and corresponding results of

the first set of sputum specimen collected.

(8) Date and results of sputum collection in TB symptomatics who had doubtful smear results

on the first examination

(9) Date (mm/dd/yr) patient was referred for an X-ray examination

(10) Date (mm/dd/yy) when X-ray result was received by DOTS facility staff and the results

(11) TB Case Number for patients who have been diagnosed with TB and registered

(12) Any significant information pertaining to symptomology and referral or diagnostic findings,

such as “patient with massive hemoptysis, referred to hospital”

Note: Target Client List (TCL) may be used as TB Symptomatic Masterlist in Public DOTS facilities.

(2) Date (mm/dd/yr) the TB symptomatic was discovered.

(3) Patient’s full name (family name written first in bold capital letters, followed by first name)

(4) Patient’s full address, including landmarks/telephone number (if possible) so the patient

can be traced in case he/she does not return to get his/her examination results

Following are the information needed on each item in the upper portion of the NTP Laboratory Request

Form for DSSM (to be filled out by the DOTS facility staff):

(1) Name of DOTS facility (BHS/RHU/PPMD/hospital) where sputum specimen was collected

(2) Date (mm/dd/yr) when sputum specimens were sent to the laboratory/microscopy unit

(3) Patient’s full name (family name first, followed by first name)


(5) Patient’s sex (Check M for male and F for female)

(6) Patient’s full address, including landmarks/telephone number (if possible) so the patient can be

traced in case he/she does not return to get his/her examination results

(7) Disease Classification: Check Pulmonary box if patient is a pulmonary TB suspect or the Extra-

Pulmonary box for TB of organs other than the lung, i.e., pleura (TB pleurisy), bones, genito-urinary

tract, etc., and the site (Specify the affected site).

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2. NTP Laboratory Request Form for DSSM

This form is accomplished by the DOTS facility staff when he/she requests for DSSM (diagnosis

or follow-up). All specimens should be sent, together with this NTP Laboratory Request Form for

DSSM, to the microscopy center. The accomplished form should be returned immediately to the

referring unit with corresponding results from the medical technologist/microscopist.

NTP Laboratory Request Form for Direct Sputum Smear Microscopy(Upper Portion)

To be filled out by Health Worker

Name of Collection unit: Date of Submission:

Name of Patient: Age Sex M F

Address (in full)

Disease Classification: Pulmonary Extra-pulmonary Site:

Reason for Examination: Diagnosis Follow-up

TB case No.

Signature of Speciment Collector: Designation of Specimen Collector:

(Signature over Printed Name)

(Be sure to enter the patient’s TB case No. for follow-up of patient’s Chemotheraphy)

Specimen Date of Collection

123

1110

9

8

7

6

3

1 2

4 5

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(8) Reason for examination: Check Diagnosis Box for sputum specimen collected for diagnosis from

tuberculosis symptomatic (three-specimens). Check Follow-up Box to follow up smear status of

patients under treatment (one specimen) and write the TB case number.

(9) Date when each of the sputum specimens was collected [Date of collection of each sputum

specimen should correspond with number on the sputum container label: for diagnosis (three

specimens); for follow-up (one specimen)].

(10) Name and signature of Sputum Collector

(11) Designation of Specimen Collector

TO BE FILLED UP BY MEDICAL TECHNOLOGIST or MICROSCOPIST

SPUTUM MICROSCOPY RESULTS

Date Received:

Laboratory Serial No:

Date of Examination: Examined by:

The completed form (with results) should be sent to the treatment unit to record the results on theNTP Treatment Card and TB register.

NTP Laboratory Request Form for Direct Sputum Smear Microscopy(Lower Portion)

(Signature over Printed Name)

2

1

* Specimen Numbers 2 & 3 = not applicable if sputum follow-up** Muco-purulent, blood stained, saliva, etc.

1 2* 3*

3

4

5

6 7

Following are the information needed in the lower portion of the NTP Laboratory Request Form for

DSSM (to be filled out by the NTP medical technologist or microscopist):

(1) Date when sputum specimen was received with this form at the laboratory or microscopy

center

(2) Laboratory serial number assigned for every examination made, whether for

diagnosis or follow-up.

Specimen Number

Visual Appearance**

Reading

Lab. Diagnosis

57

(3) Visual appearance of each specimen submitted (Quality of the specimens collected may

affect quality of the examination.) (For visual appearance of the specimens, use the

abbreviation M for muco-purulent, S for salivary, or QNS for inadequate specimen.)

(4) Readings of each specimen examined for DSSM based on this grading scale:

0 - no AFB found in 300 OIF

+n - 1 – 9 AFB in 100 OIF

1+ - 10 – 99 AFB in 100 OIF

2+ - 1 – 10 AFB/OIF in at least 50 visual fields

3+ - >10 AFB/OIF in at least 20 visual fields

(5) Over-all evaluation of specimens submitted for DSSM (A positive result should have at least

two specimens positive. A negative result should have at least three specimens negative.

A doubtful result has only one specimen positive.)

(6) Date when the specimens were examined

(7) Name and signature of medical technologist or microscopist who examined the sputum

specimen

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Following are the information that need to be recorded in the NTP Laboratory Register (to be filled

out by the medical technologist or microscopist):

(1) Laboratory serial number assigned for every examination made, whether for diagnosis or forfollow-up

(2) Date when first sputum specimen was received by the microscopy center(3) Patient’s full name (family name first in bold capital letters, followed by first name)(4) Patient’s age in years(5) Patient’s sex (M for male and F for female)(6) Name of DOTS facility where sputum for diagnosis was collected or name of treatment unit

for patients on follow-up(7) Patient’s full address, including landmarks or telephone number (if available)(8) Reason for examination: for diagnosis or follow up (Write TB case number if examination is

for follow-up.)(9) Date of examination (mm/dd/yy) and results of each sputum specimen examination(10) Significant information pertaining to the examination, i.e., positive, negative, doubtful, muco-

purulent, salivary, or inadequate specimen(11) Name and signature of medical technologist or microscopist who examined the sputum

specimens(12) Summary of DSSM results for diagnosis and follow-up should be done on every page.

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3. NTP Laboratory Register

This register, which contains all information on DSSM done by the medical

technologist/microscopist on TB symptomatics and TB patients undergoing treatment, is used in

validating microscopy data recorded on the TB Register. The medical technologist/microscopist

shall maintain this register at the microscopy center.

For Diagnosis

No.of patients on follow-upwith positive result

For Follow-up

No. ofsymptomatics

examined

No. of symptomatics with3 sputum specimens

examined

No. of symptomaticsdiagnosed as sputum

smear-positive

No. of patients onfollow-up

Summary of DSSM (12)

NTP LABORATORY REGISTER

LabSerialNo.(1)

Date ofRegis-tration

(2)

Name(3)

Age(4)

Sex(5)

Name ofCollection/Treatment

Unit (6)

Address(7)

Reason forExamination (8)

Date ofExamination/

Re-marks(10)

Sig. ofMT/Microsco

pist(11)DX F-up (TB

case no.)1st 2nd

Result (9)

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4. NTP Treatment Card

All TB patients on treatment should have an NTP Treatment Card. This card contains all the

necessary information about the TB patient, the treatment he/she is receiving, drug intake and

collection, and results of DSSM done. The NTP Treatment Card is maintained and updated by the

DOTS facility staff at the DOTS facility where the patient is receiving treatment.

NTP Treatment Card

TB CASE NUMBER DATE THE CARD ISOPENED

Month day year

REGION &PROVINCE

NAME OF DOTS FACILITY

NAME OF PATIENT OCCUPATION AGE SEX Contact Number

ADDRESS BCG Scar[ ] Yes [ ] No [ ] Doubtful

HISTORY OF ANTI-TB DRUG INTAKE: [ ] No [ ] Yes

Duration: [ ] less than 1 mo. [ ] more than 1 mo.

Specify drugs:

When: Where: Smear Status:

CLASSIFICATION OF TB:

[ ] PULMONARY

[ ] EXTRA-PULMONARY site:

TYPE OF PATIENT:

[ ] New [ ] RETURN AFTER DEFAULT (RAD)

[ ] RELAPSE [ ] TREATMENT FAILURE

[ ] TRANSFER- IN [ ] OTHER

SPUTUM EXAMINATION RESULTS/WEIGHT RECORD

Month Due Date Date Examined Result Weight(kg)

023456

>7

Chest X-ray result (if applicable): TBDC Findings and recommendations:

Category (encircle):I. 2HRZE/4HR

New Case

1. Smear (+)

2. Seriously III

2.1 Smear (-): with extensive

parenchymal lesion

as assessed by the TBDC

3. Extra-pulmonary

II. 2HRZES/1HRZE/5HRE1. Relapse

2. Treatment Failure

3. Return After Default (RAD)

4. Other (smear+/-)

III. 2HRZE/4HR

New Case

1. Smear (-): with Minimal extensive

parenchymal lesion

as assessed by the TBDC

TREATMENT OUTCOME:

NAME/RELATIONSHIP/ADDRESS OF CONTACT PERSON

SOURCE OF PATIENT

NAME OF REFERRING PHYSICIAN

[ ] Public [ ] Priviate

Contact Number of Responsible Person

12

3 4

56 7 8 9

10 11

12 13No. of House HoldContacts:

( ) <10 yrs old

( ) > 10 yrs old

14

15

16 17

18

19

20

TREATMENT STARTED: month day year

[ ] FAILED Date: / /[ ] DEFAULTED Date: / / Specify:[ ] TRANSFERED OUT Date: / /Specify:

[ ] CURED Date: / /[ ]TREATMENT COMPLETED Date: / /[ ]DIED Date: / / Cause:

Name of Treatment Partner: Designation of Treatment Partner:

21 22

23

24 25

26 27

REMARKS:

28

29

30

Drug intake (intensive phase)

Month 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 18 20 21 22 2324 25 26 27 28 29 30 31Doses

Given forthis Month

CumulativeDoses Given

Drug intake (Continuation phase)

Month 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 18 20 21 22 2324 25 26 27 28 29 30 31Doses

Given forthis Month


Following are the information that needs to be recorded on the form (to be filled out by the nurse or

designated DOTS facility staff):

(1) TB Case Number assigned to a TB case from the TB register

(2) Date when NTP Treatment Card was opened

(3) Name of region and province where the treatment facility is located

(4) Name of DOTS facility where patient is receiving TB treatment

(5) Patient’s full name (family name first in bold capital letters, followed by first name)

(6) Patient’s occupation



(9) Patient’s contact number (if available)

(10) Patient’s full address, including landmarks

(11) Presence/absence of BCG scar on patient

(12) Name/relationships/address of a person who can assist the patient for regular treatment during

the entire treatment course

(13) Contact number of responsible person

(14) Source of patient whether from the private or public sector. For private-initiated PPMD units, all

patients registered in their facility for treatment is considered private. For public-initiated PPMD

units and public DOTS facilities, private refers to patients referred by private referring physicians

and public refers to all walk-in patients or those referred by government physicians and hospitals.

(15) Name of referring physician

(16) History of patient’s previous TB treatment (If patient has had previous TB treatment history, mark

Yes and mark whether it is less than a month or more than a month. Specify drug administered

to patient, year, and place where the patient received anti-TB drugs. Include also the result of the

DSSM, if known. )

(17) Number of persons living with the patient, aged below 10 years old or 10 years old and above

(18) Patient’s classification (pulmonary or extra- pulmonary TB)

(19) Type of patient based on previous TB treatment history and results of DSSM before treatment

(New, Relapse, Transferred In, Return After Default, Treatment Failure, Other).

(20) Category of Treatment. Encircle the category of treatment regimen that will be given to the patient.

(21) Sputum examination results/Weight record. Month 0 pertains to the DSSM result before treatment.

Indicate date patient was examined and the DSSM result before treatment in the columns designated.

For the results, write the highest grading among the three specimens examined. The Due Date

for follow-up DSSM, Date Examined when the sputum examination is actually made, and Result

of the follow-up sputum examination should be noted down carefully in the columns of Month 2

to Month 7 according to the schedule of follow-up DSSM. In the last column, write patient’s weight

in kilograms during follow-up DSSM.

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(22) Date (mm/dd/yy) when first dose was actually taken by patient

(23) Treatment Outcome: Cured, Treatment Completed, Died, Failed, Defaulted, Transferred Out. Date

is when the patient stopped taking medicines.

(24) Result of patient’ chest x-ray

(25) TBDC findings and recommendations

(26) Name of treatment partner assigned to patient

(27) Designation of treatment partner: PHN, RHM, BHW or FM

(28) Drug intake during the intensive phase. Write the month when the patient started treatment in the

first column and initial the corresponding day of drug intake. The treatment partner will place his

initials in the corresponding column for the day the treatment was directly observed. X will be

drawn in the box if the patient missed taking the drugs. If the drugs will be self administered by

the patient draw a horizontal line. At the end of the month count the total number of doses given

to the patient and write in the corresponding column. The last column is the cumulative count of

the total number of doses given to the patient. This will facilitate the counting of the doses that the

patient still needs to take to complete the intensive phase of treatment.

(29) Drug intake during the continuation phase. Fill up this table in the same manner as in filling up the

intensive phase of treatment.

(30) Record pertinent information that occurred during the treatment course, i.e., adverse reactions and

reasons for failure to follow-up or defaults tracing action done.

5. NTP Identification CardAll TB patients should be issued an NTP Identification card. This is a source of informationon the patient‘s diagnosis, treatment regimen, schedule of drug-taking, and DSSM results.Both the TB patient and the treatment partner should have a copy of the NTP ID card.The treatment partner initials the NTP ID Card each time he/she sees the patient takehis/her drugs. The treatment partner keeps and maintains the NTP ID card to monitor thepatient’s drug compliance.

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Disease Classification[ ] Pulmonary[ ] Extra-pulmonary Site

Category [ ] I [ ]II [ ] IIIDate Treatment started

Mo. Day Year

Type of Patient[ ] New [ ] Treatment Failure[ ] Relapse [ ] Return after Default[ ] Trans-in [ ] Other

10 11 12

Sputum Examination Results/WeightSchedule

Date of exam

Result

Weight

BeforeTx

1mo

2mos

3mos

4mos

5mos

6mos

>7mos

13

Drug intake (Intensive phase)

Month 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 18 20 21 22 2324 25 26 27 28 29 30 31Doses

Given forthis Month


Drug intake (Continuation phase)

Month 1 2 3 4 5 6 7 8 9 10 11 12 13 14 15 16 17 18 18 20 21 22 2324 25 26 27 28 29 30 31Doses

Given forthis Month


14

15

NTPIdentification Card

TB Case No.

Mga Paalala1. Ang TB ay nakakahawa pero nagagamot.2. Ang mga gamot ay kailangan araw-araw

na inumin upang tuluyang gumaling.3. Kailangang magpasuri ng plema sa

itinakdang araw ng health worker upangmalaman kung gumaling na.

4. Kapag magaling ka na higit kangmakakatulong sa iyong pamilya atkabarangay.

Name of DOTS facility:

Name of Patient:

Address:

Treatment Partner/s:

1

2

3

4

5

Certification

Physician(Signature over Printed Name)

This certifies that the patient,

bearer of this NTP ID card, has beenCURED (completed the required treatment,

daily supervised by the healthpersonnel/BHW of

RHU/HealthCenter and, with negative smear follow-up

result at the end of the treatment).

Issued this day of , 20

6

7

8

9

(1) TB Case Number assigned to a TB case from the TB register

(2) Name of health facility/treatment unit where patient is receiving TB treatment

(3) Patient’s full name (family name first in bold capital letters, followed by first name)

(4) Patient’s full address, including landmarks/telephone number (if available) to easily trace him/her

(5) Treatment partner’s full name (family name first in bold capital letters, followed by first name)

(6) Name of the patient

(7) Name of DOTS facility where the patient is taking his/her treatment

(8) Date when the patient was declared cured

(9) Name of the DOTS facility physician

(10) Disease classification (Check if pulmonary or extra-pulmonary. Specify site.)

(11) Prescribed treatment regimen and exact date when treatment started (mm/dd/yr)

(12) Type of patient (Check if New, Relapse, Transfer-in, Treatment Failure, Return After Default, or

Other.)

(13) Data on all DSSM done. (Indicate date when the DSSM was done. For the results, write the highest

grading among the three smears examined. Specify patient’s weight in kilograms during follow-

up DSSMs.)

(14) Drug intake during the intensive phase. Write the month when the patient started treatment in the

first column and initial the corresponding day of drug intake. The treatment partner will place his

initials in the corresponding column for the day the treatment was directly observed. X will be drawn

in the box if the patient missed taking the drugs. If the drugs will be self administered by the patient

draw a horizontal line. At the end of the month count the total number of doses given to the patient

and write in the corresponding column. The last column is the cumulative count of the total number

of doses given to the patient. This will facilitate the counting of the doses that the patient still needs

to take to complete the intensive phase of treatment.

(15) Drug intake during the continuation phase. Fill out this table in the same manner as in filling up

the intensive phase of treatment.

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6. TB Register

This register gives information on the type and classification of TB cases, treatment regimen,

DSSM results, and treatment outcome of all patients registered in the DOTS facility. The nurse at

the DOTS facility maintains this register. This is one of the main sources of data in the calculation

of case detection rate, cure rate, and other program indicators.

New SmearPositive

Relapse Trans-in Return AfterDefault

TreatmentFailure

Other SmearNegative

EPPositive Negative

M F M F M F M F M F M F M F M F M F

TB REGISTER

DATE OFREGISTRA

TION(1)

TBCASE NO.

(2)

NAME

(3)

AGE

(4)

SEX

(5)

ADDRESS

(6)

HEALTHFACILITY

(7)

Name ofReferringPhysician

(9)Pub Pri

CLASS OFTB DIAG.

(P/EP)(10)

TYPE OF PATIENT (11)

New Re-lapse

Trans.

In

Re-turnafter

default

TreatmentFai-lure

Other

CATE-GORY

(12)

Source ofPatient (8)

Year:

Total Number of Patients under the following Categories

Category I Category II Category III

(13)

(13)

Following are the information that needs to be recorded on the form (to be filled out by nurse):

(1) Exact date when the patient was registered in the TB Register

(2) Case Number assigned to a TB case after registration

(3) Patient’s full name (family name first in bold capital letters, followed by given or first name)



(6) Patient’s complete address, including phone number and nearest landmark, if available, to easily

locate patient

(7) Name of DOTS facility or treatment unit where the patient is receiving treatment

(8) Source of Patient wheather from the private or public sector. For private-initiated PPMD units,

all patients registered in their facility for treatment is considered private. For public-initiated PPMD

units and public DOTS facilities, private refers to patients referred by private referring physicians

and public refers to all walk-in patients or those referred by government physicians and hospitals.

(9) Name of referring physician

(10) Disease classification: “P” for Pulmonary TB, “EP” for Extra-Pulmonary TB

(11) Type of patient under the appropriate column provided

(12) Prescribed treatment regimen by Category: I, II, III

(13) Summary of the different types of TB patients and category of treatment regimens should be done

on every page.

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Following are the information needed for each item on the TB Register (to be filled out by the nurse):

(13) Date when patient first started treatment

(14) DSSM done (Indicate date of examination in the upper row, examination results in the middle row,

and weight in kilogram in the lower row.)

(15) Appropriate treatment outcome and exact date (mm/dd/yr) when patient stopped or completed

treatment or his/her last day of drug intake

(16) Treatment Partner: PHN / RHM / BHW / FM / Others

(17) TBDC review for smear-negative cases only. Write Y if case was evaluated and N if not done

(18) Remarks (Result of CXR and any information about the patient’s status or any action taken on

his/her behalf). For patients that will be re-registered write the new TB case number in the old

registration and the previous TB case number in the new registration.

(19) Summary of treatment outcome per type of patient should be done on every page.

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(19)Type of Patient Cured Tx completed Died Failed Defaulted Trans-out

New Smear-Positive

New Smear-Negative

Relapse

Treatment Failure

Return After Default

TB REGISTER

DATESTARTED

TX (13)

SPUTUM EXAMINATION RESULTS/WEIGHT RECORD (14)

(upper space: date of exam / middlerow: results / lower space: weight)

TREATMENT OUTCOME(15)

Typeof Tx

Partner(16)

TBDCReview(Y/N)(17)

Remarks(CXR result

etc)(18)

BeforeTX.

2nd

mo. 3rd

mo. 4th

mo. 5th

mo. 6th

mo. >7th

mo. Cured TxCompl.

Died Failed Defaulted Trans Out

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7. TBDC Masterlist

This register, maintained by the TBDC secretariat, gives information on all smear-negative TB

suspects referred to and evaluated by the TBDC.

TBDC MASTERLIST

No.(1)

ReferringUnit (2)

Patient’sName (3)

PatientType(N/R)

(4)

Age(5)

Sex(6)

Occu-pation

(7)Address (8)

Dateof Refe-rral (9)

Date ofTBDC

Meeting(10)

TBDC Diagnosis (11)

Act. TB(N/R)

InactiveTB

Other LD

Tx.Category(I, II or III)

(12)

Note: Patient type (from referring unit) – write N if new and R if re-treatment; TBDC Diagnosis (1) Active TB – write N if new and R if re-treatment; (2)Inactive TB – check this column if inactive case; (3) Other Lung Disease – check this column if other lung disease; Treatment category - refersto the category of anti-TB treatment recommended by the TBDC (I, II, III).

Following are the information needed for each item on the TBDC Masterlist (to be filled out by the

TBDC Secretariat – NTP Nurse Coordinator):

(1) Serial number of patient referred to the TBDC

(2) Name of referring DOTS facility

(3) Patient’s name, family name first followed by first name and the middle initial

(4) Patient type (Write N for new case and R for re-treatment)


(6) Patient’s sex (M for male and the F for female)

(7) Patient’s occupation

(8) Patient’s exact address, including phone number and landmark, if available, to easily locate

the patient

(9) Date (mm/dd/yy) when the patient was referred to TBDC

(10) Date (mm/dd/yy) when the TBDC meeting was conducted to evaluate the patient

(11) Result of the TBDC evaluation

• If patient is with active TB, write N for new or R for re-treatment case under the

column Active TB

• If patient is diagnosed with inactive TB, put a check mark under this column

• If patient is diagnosed to have other lung disease, put a check mark under this column.

(12) Treatment Category given to the patient, if applicable.

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NTP Referral Form(Fill out in duplicate)

Please facilitate completion of treatment of patient bearing this referral form.(To be accomplished by Referring Treatment Unit)

Name of Referring Unit:Full address of Referring Unit:

Name of Patient: Age: Sex: [ ] M [ ] F Weight: Date Treatment Started

Present Address of Patient Patient’s Contact No.New Address of Patient Patient’s New Contact No.

Classification of the Patient Type of the Patient Category of Treatment[ ] Pulmonary [ ] New [ ] Relapse [ ] Category I[ ] Extra-pulmonary, [ ] Treatment Failure [ ] RAD [ ] Category II

site: [ ] Transfer-In [ ] Other (+) / (-) [ ] Category III

Remarks:

Printed Name & Signature of Referring DOTS staff

Name of Receiving Unit Telephone/Fax NumberFull address of Receiving UnitName of Patient Age: Sex: [ ] M [ ] F TB Case No.Name of Receiving DOTS Facility Staff & Signature

(Please send back a copy of this form to the Referring Unit as soon as patient has resumed treatment and registered.)

Designation

Designation

Contact/Fax number/ email address

Month/Drugs BeforeTreatment 1 2 3 4 5 6 7 8 9 10

FDC AFDC BHRZESSmear exam. result

Treatment Course and Smear Examination results

*Check the appropriate column of the number of months the drugs were taken. If drugs were taken for lessthan a month, write the number of days the patient took the drugs in the appropriate column.

Date Referred

(To be accomplished by the Receiving Treatment Unit)

Date Received:

To:

TB CASE NUMBER 1

2

3 45

6 7 8 9 1011 12

13 14

15 16 17

18

19

20 21 22

23

24 2526

27 28 29 3031 32

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Following are the information needed on each item of the NTP Referral Form (to be filled out by the

DOTS facility staff):

(1) TB case number of the patient

(2) Name of DOTS facility where the patient will be referred

(3) Name of DOTS facility where the patient is registered and receiving treatment for TB

(4) Contact/fax number or e-mail address(if available) of the DOTS facility where the patient is registered

(5) Full address of the DOTS facility where the patient is registered

(6) Patient’s full name (family name first, followed by first name)



(9) Patient’s weight in kilograms

(10) Date (mm/dd/yy) patient started on treatment as indicated in the NTP Treatment card

(11) Patient’s present complete address

(12) Patient’s contact number

(13) New address of the patient

(14) Patient’s new contact number

(15) Patient’s classification (Check if Pulmonary or Extra-pulmonary. Indicate site.)

(16) Patient’s type (Check if New, Relapse, Treatment Failure, Return After Default, Transfer-in, Other.)

(17) Appropriate treatment regimen prescribed to the patient (Check if Category I, II. or III.)

(18) Drugs prescribed for the patient and DSSM results on diagnosis and for follow-up.

(19) Any pertinent action on the patient’s referral or transfer (e.g., “transferred for continuation of

treatment” or “with massive hemoptysis, advised for hospitalization”)

(20) Person who accomplished the NTP Referral Form (printed name and signature)

(21) Designation of person referring the patient

(22) Date (mm/dd/yy) when this NTP Referral Form was accomplished

(23) Date (mm/dd/yy) the NTP Referral Form was received

(24) Name of Receiving Treatment Unit

(25) Telephone/fax number of the receiving treatment unit

(26) Full address of the receiving unit.

(27) Name of the patient



(30) New TB case number of the patient

(31) Person who accomplished the NTP Referral Form (printed name and signature)

(32) Designation of person who has received the patient

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9. TBDC Referral Form

This form gives information on the results of DSSM, chest X-ray and PE findings, history

of present illness, and history of anti-TB drug treatment. It also contains the findings and

recommendations of the TBDC. This form should be filed out by the nurse in the DOTS facility

once returned by the TBDC.

TB Diagnostic Committee (TBDC) Referral Form

(To be filled out by the referring unit)TBDC name: CHD: Province/City:Referring unit: Date of Referral:I. Patient’s DataName: Age: Sex: M [ ] F [ ]Address: Occupation:Contact Person: Relation to Patient:Address:

2. DSSM Result 1st set 2nd setDate of examinationResult

3. History of present illness (signs/symptoms), other information, and relevant physical findings Signs/symptoms and duration[ ] cough[ ] sputum production[ ] hemoptysis[ ] fever[ ] weight loss[ ] tiredness[ ] chest/back pain[ ] dyspnea

4. List any treatment taken for the present illness. State the duration of treatment.

5. History of relevant past illness (PTB and/or other diseases)

6. History of past anti-TB treatment yes [ ] no [ ]

6a. If yes, check the anti-TB drugs taken. Indicate the dates, duration of drug intake & treatment outcomesDrug Date Duration of Intake 6b. Outcome of past anti-TB treatment:[ ] INH[ ] RMP[ ] PZA[ ] EMB[ ] Strep

7. Referring unit’s clinical impression: 7a. Any treatment prescribed by referring unit:[ ] Active TB [ ] New [ ] Re-treatment[ ] Inactive TB [ ] Other (non-TB lung disease)

8. TBDC diagnosis (to be filled up by the TBDC secretariat)

8a. [ ] Active TB [ ] new [ ] re-treatment

9. TBDC recommendations (Please print; use additional pages if necessary)[ ] Anti-TB treatment Category [ ] I [ ] II [ ] III [ ] start [ ] re-start [ ] continue[ ] No anti-TB treatment[ ] Stop anti-TB treatment

Others:

10. TBDC Chairperson (for referring unit) (print and sign) 13. Received by:

11. TBDC secretariat (print and sign)

12. Date of TBDC meeting: 14. Date received:

Other signs/symptoms, duration, any important history (e.g. TBexposure, smoking history, co-existing disease, etc.)

Important PE findings:

[ ] Cured[ ] Completed[ ] Not completed[ ] Failed[ ] Not known

Remarks re: past treatment[ ] < 1 mo. [ ] 1mo or >[ ] < 1 mo. [ ] 1mo or >[ ] < 1 mo. [ ] 1mo or >[ ] < 1 mo. [ ] 1mo or >[ ] < 1 mo. [ ] 1mo or >

8b. [ ] Inactive TB 8c. [ ] Other lung disease 8d. [ ] Others

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Following are the information needed for the upper portion of the TBDC Referral Form (to be filled out

by DOTS facility staff)

TBDC Data – Name of the TBDC, the CHD and Province/City where it belongs

Data on Referring unit – Name of the Referring unit and the date (mm/dd/yy) when the referral was

made

(1) Data on patient

• Full name (family name first, followed by first name)

• Complete address

• Age in years

• Occupation

• Sex (M for male, F for female)

Data on contact person

• Full name (family name first, followed by first name)

• Complete Address

• Relation to patient

(2) Results of DSSM (Indicate results of the first and second set collection.)

(3) History of present illness (Indicate all relevant signs/symptoms and duration, as well as important

physical examination findings.)

(4) Treatment previously taken for present illness (Specify treatment and duration.)

(5) History of relevant past illness (Indicate whether or not patient has had PTB

and/or other diseases.)

(6) Past anti-TB treatment (List all treatment regimens undergone.)

(6.a) Checklist of anti-TB drugs taken (For each drug, specify date taken and duration of intake.)

(6.b) Outcome of past anti-TB treatment (Specify if: patient has been cured; treatment completed

or not completed; treatment failed; or outcome of treatment is not known. Indicate additional

remarks about previous treatment.)

(7) Referring unit’s clinical impression (Indicate whether it is active TB, inactive TB, new, re-

treatment, or other non-TB lung disease.

(7.a) Treatment prescribed by referring unit

Following are the information needed for the lower portion of the TBDC Referral Form (to be

filled out by the TBDC secretariat – NTP Nurse Coordinator):

(8) TBDC diagnosis

(8.a) Active TB (Check if new or re-treatment.)

(8.b) Inactive TB

(8.c) Other lung disease

(8.d) Others

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(9) TBDC recommendation

Specify:

• Anti-TB treatment, No anti-TB treatment, or Stop anti-TB treatment

• Treatment regimen Category I, II, or III

• Start, re-start, or continue treatment

• Write down additional impressions or instructions. Use additional page/s, if

necessary.

(10) Printed name and signature of the TBDC chairperson

(11) Printed name and signature of person responsible in the TBDC secretariat

(12) Date of TBDC meeting when referral was evaluated

(13) Printed name and signature of person in referring unit who received the accomplished

TBDC Referral Form

(14) Date (mm/dd/yy) when referring unit received back TBDC Referral Form

Table 4.1. Persons Responsible for the Recording Forms

IV. Persons Responsible for the Recording Forms

TB Symptomatics Masterlist/TBSymptomatics Target client List(optional)

Records Responsible for InitialRecording

Responsible forMaintenance and

Updating

Designated DOTS Facility Staff Designated DOTSFacility Staff

NTP Laboratory Request Form forSputum Examination

Designated DOTS Facility Staff

NTP Laboratory Register Medical Technologist andMicroscopist

Medical Technologistand Microscopist

NTP Treatment Card Nurse Designated DOTSFacility Staff

NTP Identification Card Nurse Treatment Partner

TB Register Nurse Nurse

NTP Referral Form Nurse/Physician

TBDC Masterlist NTP Nurse Coordinator

TBDC Referral Form Physician/Nurse Physician/Nurse

Nurse/Physician

NTP Nurse Coordinator

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V. NTP REPORTING FORMS

The NTP Reporting Forms consist of the following:

• NTP Quarterly Report on Laboratory Activities;

• NTP Quarterly Report on All TB Cases;

• NTP Quarterly Report on Drug Inventory and Requirement;

• NTP Quarterly Report on Treatment Outcome;

• Quarterly TBDC Accomplishment Report; and,

• EQA reports – (refer to the Manual on Quality Assurance for Sputum Smear Microscopy)

1. NTP Quarterly Report on Laboratory Activities

This report provides information on the total number of TB symptomatics’ collected

sputum specimens and the total number of smear-positive cases identified quarterly. This is

accomplished by the medical technologist or microscopist at the microscopy center of the

DOTS facility. The source of data for this report is the NTP Laboratory Register. An optional

Counting Sheet for Laboratory Activities Report is also available.

The NTP Quarterly Report on Laboratory Activities is submitted to the provincial or city

NTP Coordinators who consolidate and analyze the data. The CHD NTP coordinators collate

and analyze the data from provinces, cities and PPMD units. Collated data are then submitted

to the National Center for Disease Prevention and Control (NCDPC) of the Department of

Health.

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Quarterly Report on NTP Laboratory Activities(Source of Data- NTP Laboratory Register)

Name of Province/City:

Name of DOTS Facility:

Total population of catchment area:

TB symptomatics/patients

Examined during Quarter of

Date Reported:

Prepared by:

Designation:

Casefinding:

∗ Positivity rate is an important indicator of microscopy performance. Positivity Rate = Total no. of sputum smear positive cases x 100 Total no. of TB symptomatics examined

Laboratory activities TOTAL

1. No. of TB Symptomatics examined:

2. No. of TB Symptomatics with 3 sputum specimens:

3. No. of TB Symptomatics diagnosed as smear-positive with 2 or more positive results:

(including the number of doubtful cases in the1st collection with at least one positive resultin the 2nd collection set)

4. Positivity Rate*

5. No. of TB Symptomatics with Doubtful result:

Treatment Follow-up

6. No. of follow-up examinations done

7. Number of smear-positive cases among the follow-up examinations

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COUNTING SHEET FOR LABORATORY ACTIVITIES REPORT (Optional)_______ Quarter of _______

2. NTP Quarterly Report on All TB Cases

This report summarizes the NTP case finding on all TB cases (new smear-positive cases,

relapses, treatment failure, Return After Default, Other, smear-negative cases, and extra-pulmonary)

for monitoring and evaluation of program implementation. This is accomplished by the nurse at the

DOTS facility. Source of data for this report is the TB Register.

The NTP Quarterly Report on All TB Cases is submitted to the provincial or city NTP coordinators

who consolidate and analyze the data. The CHD NTP coordinators collate and analyze the data

from provinces, cities and PPMD units. Collated data are then submitted to the NCDPC of the DOH.

1

2

3

4

5

6

7

8

9

10

Page STARTLab.No.

TOTALPersons

No. of TBSympto-matics

Examined

No. of TBSympto-maticswith 3

SputumSpecimens

No.of TB

Sympto-matics

withDoubtfulResults

No.of TB

Sympto-matics

with 2 ormore

Positive

No.of

Follow-upExamina-

tionDone

Quarterly Report on All TB Cases (Source of Data – TB Register)

Name of CHD:

Name of PHO/CHO:

Name of DOTS facility:

Patients Registered during the Quarter of year

Date Submitted:

Prepared by:

A. All TB cases registered during the quarter:

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3. NTP Quarterly Report on Drug Inventory and Requirement

This report contains the summary of the number of cases according to category of treatment

regimen to calculate the drug requirement at the DOTS facility and provinces. Source of data

for this report is the TB register. The nurse accomplishes this report, which he/she submits to the

provincial or city NTP coordinators. The provincial and city NTP coordinators consolidate data and

submit these to the CHD NTP coordinators. The CHD NTP coordinators then consolidate and

submit report to the NCDPC of the DOH.

Name and Designation

Type ofPatient/Sex/DOTS facility

NewSmear-

Positive (1)

Relapse(2)

Trans-in (3)

RAD(3)

TreatmentFailure

(5)

Other (6)

Positive Negative

New Smear-Negative

(7)

Extra-pulmonary

(8)

Public

Private

Subtotal

Total

M F M F M F M F M F M F M F M F M F

B. Breakdown of New Pulmonary smear-positive cases by age and sex:Age-group (years)

0 - 9

M F

10 - 14

M F

15 - 24

M F

25 - 34

M F

35 - 44

M F

45 - 54

M F

55 - 64

M F

65 andabove

M F

Total

M F Total*

* Should be the same as the total in Column 1 of A

C. Treatment Regimen given:

Type of Treatment Regimen Category I Category II Category III

Cases initiated treatment

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Drug Inventory and Requirement Report (Source of Data – Quarterly Reports and Physical inventory)

I & IIIIITotal for Cat. I, II & IIITotal + Buffer(Total multiplied by 2)Available on handRe-order forCat. I, II & III

Childhood TBTotal + Buffer(Total multiplied by 2)Available on handTotal re-order

Category No. ofCases

STOP TB KitCategories

I & III

STOP TBKit

Category II

H syr(200mg/

5 ml120ml)

R syr(200mg/

5 ml120ml)

Category No. ofCases

F D C A( H R Z E )

( B P )

FDC B(HR)(BP)

E(BP)

S(vial)

H syr(200mg/

5 ml120ml)

R syr(200mg/

5 ml120ml

I & III

II

Childhood TB

Total for Cat. I, II & III

Total + Buffer(Total multiplied by 2)

Available on hand

(x 6)

(x 9)

(x 12)

(x 15) (x 10) (x 56)

Z syr(250mg/

5 ml120ml

Z syr(250mg/

5 ml120ml)

(x 7) (x 7) (x 4)

(x 7) (x 7) (x 4)

Total

4. NTP Quarterly Report on Treatment Outcome

This report contains information on the outcome of treatment for a group of patients who were

treated 13-15 months earlier. Such information serves as basis for evaluating the effectiveness of

treatment regimen. Source of data for this report is the TB register. This report is accomplished by

the nurse.

The NTP Quarterly Report on Treatment Outcome is submitted to the provincial or city NTP

coordinators who will consolidate and analyze the data. The CHD NTP coordinators will collate and

analyze the data from the provinces, cities and PPMD units. Collated data shall be submitted to the

NCDPC of the DOH.

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NTP Quarterly Report on the Treatment Outcome of Pulmonary TB Cases (Source of Data – TB Register)

Name of Region:

Name of PHO/CHO:

Name of DOTS facility :

Patients registered during the

Quarter of

Date Reported :

Prepared by :

Designation:

* Of these, ___________(number) were excluded from evaluation of chemotherapy for the following reasons:_____ Trans-in_____ Extra-pulmonary_____ Other

1. New Cases

1.1 Smear ( + )1.2 Smear ( - )

2. Re-treatment

2.1 Relapse 2.2 Treatment Failure 2.3 Return After Default

Total Number ofPulmonary TB Cases( Copy the totalnumber reported inthe Case FindingReport during thesame quarter)

Type

(1)

Cured

(2)

Com-pletedTreat-ment

(3)

Died

(4)

Failed

(5)

Defaul-ted

(6)

Trans-ferred

out

(7)

TotalNo.

Evalua-ted

Grand Total

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5. Quarterly TBDC Accomplishment Report

This report contains information on the total number of cases referred from different health

facilities and evaluated by the TBDC, with the corresponding findings and recommendations. This

serves as the basis for monitoring and evaluation of the quality of diagnosis among referred smear-

negative, X-ray positive cases. The sources of data for this report are the TBDC Referral Forms

and TBDC Masterlist. The NTP nurse coordinator accomplishes this report and submits it to the

CHD NTP coordinator. Collated reports are submitted to the NCDPC of the DOH.

QUARTERLY TBDC ACCOMPLISHMENT REPORT FORM

Name of Region:Name of the TBDC:Data for the Quarter year

Name of Province/City:Date Submitted:Prepared by:

1. Total no. of (smear-neg./X-ray pos.) TB symptomatics referred to TBDC

TBDC Diagnosis

2. Total number of active TB cases diagnosed by TBDC

2.1. Classification of active TB cases diagnosed by TBDC TB, New:

TB Retreatment:

Total:

3. Total number of inactive TB patients

4. Total number of patients diagnosed as “other lung disease”

5. Total number of patients evaluated by TBDC for this quarter

6. Total number of patients recommended by the TBDC for

anti-TB treatment this quarter

Following are the information needed in the Quarterly TBDC Accomplishment Report Form:

General Information: Name of Region and province/city and CHD, Name of the TBDC, Date (mm/dd/yy)

when the report was submitted, Quarter of the year that the data are reported and Name and Signature

of the person who prepared the report.

(1) Total number of TB symptomatics referred to TBDC.

(2) Total number of active TB cases diagnosed by the TBDC

Classification of referred TB cases diagnosed by TBDC

• Number of new TB cases

• Number of re-treatment TB cases

• Total TB cases (new + Re-treatment)

(3) Total number of inactive TB patients

(4) Total number of patients diagnosed as “Other Lung Diseases”

(5) Total number of patients evaluated by the TBDC for the present quarter

(6) Total number of patients recommended by the TBDC for anti-TB treatment in this quarter

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Logistics Management

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One of the five components of the DOTS strategy is uninterrupted supply of quality-assured

anti-TB drugs ( isoniazid, rifampicin, pyrazinamide, ethambutol, and streptomycin). Therefore all DOTS

facilities should have adequate supply of these anti-TB drugs to ensure that drugs are available when

patients need them. An adequate supply of anti-TB drugs would also result to prevention of TB transmission

and development of multi-drug resistant cases. NTP supplies should also be adequate to ensure

continuous detection of TB cases. NTP supplies include sputum cups, glass slides and slide boxes,

reagents, syringes, and recording and reporting forms.

To ensure the regular supply of anti-TB drugs and their appropriate use, each step of the anti-

TB drug management cycle must be followed (Figure 5.1). The NTP coordinators should closely monitor

the entire process even if they are not directly responsible for each step.

Figure 5.1. Anti-TB Drug Management Cycle

Management Support- information system- organization/staffing- budgeting- training

ProductSelection

Rational Use,Monitoring &Evaluation

Procurement

Distributionand Storage

I. Product Selection. Product selection is the process of establishing a limited list of essential anti-

TB drugs to be procured based on the treatment guidelines. Specifications of each drug should be

defined and should include the following: drug description; generic name; local trade name; dosage

form; strength; and package presentations.

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II. Procurement. Procurement is the process of acquiring anti-TB drugs through purchase or donation.

The process includes quantifying drug needs, selecting methods for purchasing, selecting reliable

suppliers, managing tenders, assuring quality, and ensuring compliance with contract terms.

The NTP coordinator’s contribution to procurement usually involves estimation and calculation

of the quantities of each drug needed. The NTP coordinator must also ensure that drugs and other

supplies are correctly quantified so that every TB patient can begin treatment without delay and

complete treatment without interruption. If the budget does not cover the cost of all drugs to be

procured, the quantity of drugs must be decreased according to the number of cases, since all

drugs must be available when needed by the patient.

III. Distribution and Storage. Distribution is the process by which procured anti-TB drugs are received

at the port of entry, cleared through customs, and transported from the central warehouse to the

regional, provincial health offices, up to the DOTS facilities where they are dispensed to the patients.

Distribution of drugs from the time these were received at the port until these are distributed to the

different health facilities should be monitored carefully. TB drugs should be cleared rapidly through

customs to avoid deterioration in the port of entry.

Quality and quantity of TB drugs should be inspected before distribution from the receiving

warehouse. Random samples of each shipment need to be inspected to check out labeling

(language, dosage strengths, dosage form, and expiry date), quantities received, and condition

of the drugs against specifications of the contract. Random samples should be sent also to

the Bureau of Food and Drug (BFAD) for identification test to determine the content of the

active ingredient and dissolution test.

Once the drug shipment has passed quality inspection and testing, the drugs may be

distributed to and stored at local warehouses and DOTS facilities.

The following are storage procedures that will ensure that drugs and other supplies

are: a) protected from theft and unauthorized access; b) protected from heat, light, moisture/rain,

dust, pest, poison, and fire; and c) easy to find.

A. Protected from Theft and Unauthorized Access

1. Store drugs and other supplies in a secured stock room.

2. Maintain accurate and up-to-date records to ensure that if supplies are stolen,

DOTS facility workers know the missing amount from the stock. DOTS facilities

should maintain a stock card for every kind of drug or supply to monitor the amount

received and dispensed. See Form 5.1.

3. Ensure access to supplies. However, limit access to one or two persons and ensure

that one person is always available to distribute the supplies.

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Form 5.1. Sample Stock Card

Name of Item: Stop TB Kit Category I & III

Unit: Kit

B. Protected from heat, light, moisture/rain, dust, pest , poison, and fire

1. Store drugs and NTP supplies separately from office supplies, insecticides, and chemicals to

avoid contamination.

2. Store drugs in a cool place, away from direct sunlight.

3. Keep the roof in good condition to prevent leakages.

4. Store drugs and other supplies off the ground by using pallets and away from walls to reduce

moisture and to promote air circulation.

5. Keep stock room clean and well-ventilated.

6. Ensure that fire safety equipment is available and accessible.

C. Easy to Find

1. Store drugs according to their expiration date. Make sure each drug’s expiration date is marked

clearly.

2. Use FEFO ( First Expiry, First Out): First drugs to expire should be used or distributed first.

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Date

08/28/05

09/05/05

09/06/05

Description

(Received from/Issued to)

Received from CHD

Issued to PHO

Totalvalue

Quantity

In

2000

Out

500

Balance

10

2010

1510

Remarks(Expiration

date, lot no.,etc.)

08/2007, SL417

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IV. Rational use, monitoring, and evaluation. Rational drug use entails correct diagnosis, followed

by correct prescribing, labeling, dispensing, and ensuring that patient adheres to recommended

treatment regimens. Fixed Dose Combinations promote good practices; these can contribute to

fewer prescribing and dispensing errors because there are fewer tablets to handle at any one time.

Use of TB kits assures the availability of drugs for the entire duration of treatment. However, the

use of TB kits does not replace DOT.

Drug logistics cycle should be monitored regularly to ensure that the right quantities of anti-

TB drugs are available when needed.

Procurement of anti-TB drugs shall be done annually through public bidding.

Under the National Tuberculosis Control Program, the DOH Central Office shall procure the drugs

and NTP supplies because these cost less with bulk purchase.

Once the drugs have been delivered, inspected, and analyzed for quality by the Bureau of

Food and Drug, these will be sent to the Centers for Health Development for distribution to the

different provinces and cities. The provincial LGUs then will distribute the drugs to the different

DOTS facilities. Drug requirements of the DOTS facilities will be based on their usage for the past

quarter. The DOTS facilities must submit the NTP Quarterly Report on Drug Inventory and

Requirement regularly to the provincial/city NTP Coordinator. The consolidated data will then be

submitted to the CHD NTP Coordinator.

The quantity of drugs to be requested is determined through the following computations,

depending on the drug preparation to be procured -- either TB kits, blister packs of FDC or SDF:

A. Stop TB Kits (Table 5.1)

1. Count the number of patients registered in the previous quarter per category.

2. Compute the quantity of TB drugs required per category. For Stop TB kits, the total

number of Stop TB kits required is equal to the total number of patients per category. For

FDC and SDF blister packs and SDF tablets, the total quantity of drugs required depends

on the factor to be multiplied with the number of patients per category (See Tables 5.1,

5.2, 5.3, & 5.4).

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Table 5.1. Computation for Quarterly Drug Requirement for Stop TB Kits

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B. Blister Packs of Fixed Dose Combination Drugs (FDCs)

Table 5.2. Computation for Quarterly FDC BP Drug Requirement

Category

Category I

Category II

Category III

Total

Stock with Buffer

Stock on Hand

Total Kits to be requested

No. of cases

No. of cases

Total kits required x 2

No. of cases

Total kits required x 2

Stop TB Kit for Cat Iand III

Stop TB Kit for Cat II

No. of cases X 6

No. of cases X 9

No. of cases X 6

Total BP x 2

FDC- A

(BP)

No. of cases X12

No. of cases X 15

No. of cases X 12

Total BP x 2

FDC- B

(BP)

No. of cases X 10

Total BP x 2

ETHAMBUTOL

(BP)

No. of cases X 56

Total BP x 2

STREP-

TOMYCIN

Total BP to be

requested

Category

Category I

Category II

Category III

Total

Stock with Buffer

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C. Single Drug Formulation (SDF)

Table 5.3.a Computation for Quarterly SDF BP Drug Requirement

Table 5.3.b Computation for Quarterly SDF Tablets Drug Requirement

Category Isoniazid

(400 mg/tab)

Rifampicin

(400mg/cap)

Ethambutol 400

mg/tab

SM

(1 gm/vial)

No. of

cases x 168

No. of

cases x 168

No. of cases x 112

No. of

cases x 224

No. of

cases x 224

No. of cases x 448 No. of

cases x 56

No. of

cases x 168

No. of

cases x 168

No. of cases x 112

TOTAL

Pyrazinamide

(500mg/tab)

No. of

cases x 112

No. of

cases x 168

No. of

cases x 112

Stock withBuffer

Total x2 Total x2 Total x2 Total x2Total x2

Stock onHand

Total drugsto berequested

Category SCC I

(HRZ) BP

SCC II

(HR) BP

Ethambutol 400

mg/tab

SM

(1 gm/vial)

No. of cases x 8 No. of cases x 16 No. of cases x 112

No. of cases x 12 No. of cases x 20 No. of cases x 448 No. of cases x 56

No. of cases x 8 No. of cases x 16 No. of cases x 112

TOTAL

Stock with Buffer Total BP x 2 Total BP x 2 Total tablets x 2 Total vials x 2

Stock on Hand

Total BP to berequested

Category I

Category II

Category III

Category III

Category II

Category I

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3. Multiply by 2 the quantity of drugs required to get the total stocks needed. This already includes the

buffer stock.

4. Count the stocks on hand and subtract total from the total stocks required. The difference will be

the quantity of drugs to be requested.

5. Submit the NTP Quarterly Report on Drug Inventory and Requirement, together with other NTP

quarterly reports every first week of the succeeding quarter, to the provincial/city NTP coordinators

who will then submit the report to the CHD NTP coordinator.

6. Buffer stocks must be maintained at all levels to avoid stock-outs. The adequate reserve level must

be as follows:

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The LGUs are tasked to procure drugs for Category III patients and for patients who will develop

adverse reactions to FDC drugs. The LGUs are also encouraged to procure other supplies to support

local TB activities

Level Buffer Stock

DOH / CHD Six months

Province/City Three months

DOTS Facility Three months

The following tables will guide the NTP coordinator in estimating the NTP supplies

required by the DOTS facilities.

Table 5.4. Computation for Annual Estimated Supplies for DSSM

*(Total population x 133/100,000) x 75%

Expected

Sm (+) identified*

No. of Examination

For Diagnosis For Treatment

Total

A B (A x 10X3) C (A x 3) D (B+C)

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Table 5.5 Computation for Annual Estimated Recording and Reporting Forms

*Basis for this computation will be the previous year’s annual accomplishment.

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Microscopy Supplies Unit of measurementrequired per item

Sputum cups, 1,000/box

Number of boxes/bottles required

D x 1 pc D/1,000

Glass slides, 72 pcs/box D x 1 pc D/72

Immersion oil, 100cc/btl D x 0.15 cc D/770

Pre-mixed, Hot stain

Carbol Fuschin

Acid Water

Acid alcohol

Methylene blue

D x 4 cc

D x 8 cc

D x 4 cc

D x 2 cc

D/500

Name of Form and Record

NTP Laboratory Request form for DSSM

NTP Laboratory register

Treatment Card

ID Card

TB Register

Quarterly Report on Laboratory Activities

Quarterly Report on New Cases and Relapses

Quarterly Report on Treatment Outcome

NTP Referral Form

TBDC Referral Form

Quantity Needed for eachDOTS Facility

1 per patient

1/500 patients

1 per patient

2 per patient

1/200 patient

12 per year

12 per year

12 per year

3% of the new smear positive cases

37% of smear positive cases

Table 5.4 (Cont.)

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Monitoring is an on-going process of collecting and analyzing information about program

implementation. It involves: a) regular assessment of whether or not activities are being carried out as

planned and how these activities are being done; and b) identifying problems and implementation

bottlenecks. Data and information gathered through monitoring should be immediately processed,

analyzed, and disseminated to stakeholders who can make the best use of such.

Supervision is an essential management tool to ensure that implementers carry out the program’s

policies, standards, and procedures correctly, effectively, and efficiently. It is also an opportunity for

supervisors to do the following:

1. Discuss with DOTS facility staff important issues related to the program;

2. Check records and reports;

3. Acknowledge and reinforce good performance;

4. Help DOTS facility staff identify and correct inadequacies or weaknesses in

performance;

5. Give feedback and solicit ideas on how to improve program implementation;

6. Provide exit feedback with corresponding recommendations about problems identified to improve

program implementation; and

7. Provide on-the-job training.

Evaluation is the regular assessment of the process or development of any given

program or project with particular focus on its effectiveness and impact. This process is carried out

by each of the NTP coordinators by analyzing indicators, data, and relevant information from records,

reports, and feedback from field health implementers, surveys, and studies done by other agencies.

Monitoring and evaluation ideally go hand-in-hand. While monitoring entails observation and

description of how the project/program is being conducted, evaluation involves interpretation of results

or change over time. The question in monitoring is: Are things going all right? The question in evaluation

is: So, did it work?

Monitoring, Supervision, and Evaluation

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Monitoring and evaluation together can enable program implementers to:

• Better understand how the program is working;

• Make informal decisions regarding operations;

• Ensure most effective and efficient use of resources;

• Look at the extent to which the program/project is having or has had the desired impact; and

• Fine-tune future program impact.

I. OBJECTIVES

A. Ensure that program implementers adhere to NTP policies and guidelines.

B. Monitor progress of program implementation and identify areas of improvement to maintain

quality DOTS implementation.

C. Evaluate NTP activities to determine if program targets of 70 percent case detection rate and

85 percent cure rate are reached and maintained. Identify problems and recommend and

institute possible solutions.

II. POLICIES

A. The provincial or city NTP coordinators shall serve as NTP supervisors at the RHU or MHC

level. They shall be responsible for: 1) regular monitoring (at least quarterly) of DOTS facilities,

hospitals, PPMDs, and all other certified DOTS centers; and 2) evaluating progress and

performance of NTP. In coordination with the DOH/CHD NTP coordinators, they shall see to

it that DOTS facilities operate in accordance with NTP directions, standards, and technical

policies.

B. The following shall serve as NTP supervisors at specific levels: municipal health officer at the

RHU; PHN at the BHS; PPMD physician at the PPMD unit; and chief of hospital at the hospital.

MHOs shall also visit the BHS to maintain good working relationships between the coordinators

and the health workers. Frequency of visit will depend on the BHS’ level of performance, as

well as that of the health workers.

C. With the Quality Assurance System as guide, the CHD/PHO/CHO shall monitor regularly (at

least quarterly) the performance of laboratory services and functionality of the TB Diagnostic

Committee.

D. The health staff concerned with NTP at each level shall regularly analyze data from quarterly

reports using standard program indicators and provide feedback of findings with corresponding

recommendations to the staff or authorities concerned.

E. Continuous advocacy efforts to secure commitment of LGUs to counter-share in the purchase

of anti-TB drugs and other supplies shall be undertaken.

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Reports include: a) Quarterly Report on all TB cases; b) Quarterly Report on the Treatment Outcome;

c) Quarterly Report on NTP Laboratory Activities; d) Drug Inventory and Requirement Report; and, e)

Quarterly Report on External Quality Assessment (Refer to Manual on Quality Assurance for Sputum

Smear Microscopy).

III. PROCEDURES

A. Monitoring and Supervision Activities

Identify areas to be visited and determine frequency of visits. Those with problems should be

visited more frequently. Use the following guidelines for supervisory visits:

1. Compare and verify that all information in the following records are accurate and consistent:

• TB Register with NTP Laboratory Register (Verify that all smear positives in the NTP

laboratory register are registered and started on treatment in the TB register. Verify

also that smears of patients for DSSM follow-up are examined and are on time.)

• TB Register with NTP Treatment Cards

• NTP TB Laboratory Register with NTP Treatment Cards

Figure 6.1 Flow of Reporting

DOTS Facilities

PHO/CHO

CHD

NCDPC - DOH RCC-PPMD

Partner Agencies

Data Collection and Analysis First week of the quarter

Data collection, consolidation,analysis and feedback Second week of the quarter

Third week of the quarterData collection, consolidationanalysis and feedback

Data collection, consolidationanalysis and feedback

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2. Review NTP treatment cards. Check for the following:

• There is a TB case number

• Type and classification of patient is correct

• DSSM was done for diagnosis and follow-ups are on time

• Category of treatment regimen is correct

• Intensive phase is extended for patients that are still smear positive at the end of the

intensive phase

• Drug intake is complete

• Treatment outcome is correct

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3. Review TB Register. Check for the following:

• TB case number

• Type and classification of patient is correct

• DSSM results on diagnosis is done and follow-up is done on time

• Conversion rate at the end of the second or third months of treatment

• Treatment outcome is correct

4. Review NTP Laboratory Register. Check for the following:

• TB case number of patients for the follow-up examination are written

• Rate of three sputum specimen collections is more than 90%

• Positivity rate is between 10 to 20 percent

5. Observe DOTS facility staff are giving correct and relevant health education to the patients

and DOT is done correctly

6. Interview DOTS facility staff and patients

7. Conduct physical inventory of NTP drugs and other supplies.

Coordinators/supervisors must share all relevant information and recommendations

arising from the visits, preferably in writing, with DOTS facility staff concerned. Courses of

action to address deficiencies, mistakes, and acts of carelessness must be discussed and

solutions agreed upon by both supervisor and the concerned DOTS facility staff. For further

details on Monitoring and Supervision, please refer to Handbook for Quality DOTS: Pointers

to Improve Monitoring and Supervision.

B. Evaluation

1. The nurse or the designated DOTS facility staff prepares, during the first week of each quarter,

the Quarterly Report on All TB Cases registered during the previous quarter and the Quarterly

Report on the Treatment Outcome of Pulmonary TB Cases registered in the same quarter

last year. While the medical technologist/microscopist prepares the Quarterly Report on NTP

Laboratory Activities of the cases registered during the previous quarter. The physician analyzes

all quarterly reports to evaluate the performance of the DOTS facility. The DOTS facility staff

submits the reports to the provincial/city NTP coordinator.

All DOTS facility staff concerned evaluate their performance by analyzing indicators, such

as the following: a) three-sputum collection rate; b) positivity rate; c) proportion of pulmonary

smear-positive cases out of all pulmonary cases; d) case detection rate of new smear- positive

cases; e) case notification rate of new smear-positive cases per 100,000 population; f) sputum

conversion rate at the end of two or three months of treatment for new smear-positive cases; and

g) cure rate of new smear-positive cases.

The provincial/city coordinator should disaggregate the reports of PPMD units to reflect the

additionality of cases in the city/municipality where PPMD is implemented.

2. The source of data for the laboratory activities is the NTP Laboratory register while source

of data for the Quarterly report on All TB cases and Treatment Outcome is the TB register.

Therefore, the information in the report is only as accurate as the information recorded in the

TB Register and the NTP Laboratory Register. The quarterly reports are based on the following

coverage period:

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The provincial/city NTP coordinators collect, consolidate and analyze all quarterly reports

from the implementing DOTS facilities. The CHD NTP coordinators send the data, consolidated

by province, city, PPMD units, Hospitals, NGOs, etc. from all Quarterly Reports, to the NTP

manager for consolidation and analysis. Recommended courses of action anchored on relevant

findings, based on program indicators (see Table 6.1) gathered from the quarterly reports, should

be used and applied to ensure effective implementation of the TB control program.

IV. MONITORING FORMS

Standardized monitoring tools/checklists based on the program indicators established

shall be used in monitoring, supervision, and evaluation activities.

January 1 – March 31

April 1 – June 30

July 1 – September 30

October 1 – December 31

1st

Quarter

2nd

Quarter

3rd

Quarter

4th

Quarter

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NTP MONITORING TOOL

Date:CHD: Province:Monitoring Team:

POPULATION (Current year)Period (Quarter) MonitoredI. CASEFINDING (Lab. Register)A. No. of TB Symptomatics examinedB. No. with 3-sputum specimen Per cent with 3-Sputum SpecimenC. No. who are Smear (+) Positivity RateII. CASEHOLDING (TB Register/ Treatment Card)A. Total no. of Patients Initiated Tx 1. Pulmonary: a. New smear (+) b. New smear (-) Cat I Cat III c. Relapse d. Treatment Failure e. Other retreatment 2. Extrapulmonary % of smear (+) to Total PTB Case Notification Rate Case Detection RateB. Sputum Conversion 1. No. New Sm(+) due to undergo sputum examination at 2 mos. 2. No. who underwent sputum exam at 2 mos. 3. No. who converted Efficiency rate = 3/1 (Converted/due) Efficacy rate = 3/2 (Converted/examined)C. DOTS Implementation1. Total No. of Patients under DOTS2. No. Health Worker as partners3. No. BHW/BNS as partners4. No. Other community volunteers5. No. Family Member as partnersDOTS Implementation Rate

Monitoring Indicators Facility Facility Facility Facility

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Monitoring Indicators Facility Facility Facility Facility

D. TREATMENT OUTCOME1. New Smear (+)Total No. initiated treatmentCuredCompleted TreatmentDiedFailedDefaultedTransferred Out2. RelapseTotal No. initiated treatmentCuredCompleted TreatmentDiedFailedDefaultedTransferred Out3. New Smear (-)Total No. initiated treatmentCompleted TreatmentDiedFailedDefaultedTransferred OutQuality Assurance - LaboratoryTotal No. of errorsMajor errorMinor errorQuantification error(See other monitoring forms in the Manualof Quality Assurance of Sputum SmearMicroscopy - Forms 3, 6, & 7)TBDCA. Total No of Smear(-) C-Xray positive TB

evaluated by TBDCB. No. of Sm(-), CX-ray (+) confirmed as

active and recommended by TBDC fortreatment

Proportion of Sm(-), CX-ray (+) TB casesconfirmed as active TB & recommendedfor Treatment

No. % No. % No. % No. %

No. % No. % No. % No. %

No. % No. % No. % No. %

No. % No. % No. % No. %

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Monitoring Indicators Facility

E. Drugs and NTP SuppliesFDC A (HRZE)FDC B (HR)PZAEthambutolStreptomycin (750mg)SlidesSputum CupsAFB StainLab request formLab RegisterTB RegisterTB Symptomatic MasterlistTreatment cardID cardsNTP Referral formsTBDC referral forms* DOE-Date of ExpirationF. LGU CommitmentA. Municipal NTP budget (amount)B. Total Health budget (amount)Proportion of Mun NTP budget tototal health budget (annualy)

C. LGU is providing TEVs/per diem forsupervision/monitoring

D. Availability of : 1. Medical Technologist 2. NTP Microscopist

G. PPMDNo. of trained referring physicians ina PPMD UnitNo. of DOTS referring physiciansreferring TB suspects for sputummicroscopyNo. of DOTS referring physiciansreferring TB cases for treatmentNumber of New Smear (+) from PPMD

H. Health PromotionNo. of advocacy activities conductedNo. of BCC materialsproduced/reproduced/distributed

DOE

Facility

DOE

Facility

DOE

Facility

DOE

Yes [ ]No [ ]

Yes [ ]No [ ]Yes [ ]No [ ]

Yes [ ]No [ ]

Yes [ ]No [ ]Yes [ ]No [ ]

Yes [ ]No [ ]

Yes [ ]No [ ]Yes [ ]No [ ]

Yes [ ]No [ ]

Yes [ ]No [ ]Yes [ ]No [ ]

No. No. No. No.

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FINDINGS:

1.

2..

3.

4.

5.

6.

7.

8.

9.

10.

RECOMMENDATIONS:

1.

2..

3.

4.

5.

6.

7.

8.

9.

10.

MONITORING TEAM MEMBERS:Date:

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Table 6.1. Program Indicators

INDICATORS CALCULATION DATA SOURCE

CASE FINDING

1. Three- sputumCollection Rate (%)

Number of TB symptomatics who submitted 3 sputum specimens

------------------------------------------------------------- x 100 Total number of TB symptomatics examined

Total number of sputum smear-positive cases discovered--------------------------------------------------------------- x 100

Total number of TB symptomatics examined

Number of New smear-positive cases detected---------------------------------------------------------------- x 100

Number of estimated new smear-positive TB cases

(The denominator is a WHO estimation for each countrybased on available data including case notifications, mortalityand studies on disease prevalence and risk of infection,and adjusted for countries with high incidence. These

estimations are reported every year by WHO in the annual“Global Tuberculosis Control” report.)

Number of New smear-positive cases notified

------------------------------------------------------------------- x 100,000

Total number of population in the specified area

Laboratory Register

Quarterly report on laboratoryActivities

2. Positivity Rate (%) Laboratory Register

Quarterly Report on Laboratory Activities

3. Case DetectionRate of newsmear-positive cases

TB Register

Quarterly Report on All TB Cases

4. Case NotificationRate of newsmear-positivecases per 100,000population

TB Register

Quarterly Report on All TB Cases

Population Statistics

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INDICATORS CALCULATION DATA SOURCE

CASE HOLDING

5. Proportion ofpulmonary smear-positive cases out ofall pulmonary cases(%)

6. Sputum conversionrate at the end of 2months of treatment for new smear-positive cases (%)

7. Treatment outcomesfor new smear-positive cases, Newsmear-negativecases, Relapsecases, Return AfterDefault andTreatment Failurecases (%). (Eachcase type is adifferent cohort).

(Reminder: There is no cure rate

applied to smear-negative

cases.)

Number of Pulmonary smear-positive cases (New and Relapse) registered

--------------------------------------------------------------- x 100 Total number of pulmonary (New smear-positive,

New smear-negative and Relapse) cases registered

Number of New sputum smear-positive cases which are smear-negative at the end of 2 months of

treatment--------------------------------------------------------------- x 100 Total number of New sputum smear-positive cases

registered during some period of time

TB Register

Quarterly Report on AllTB Cases

TB Register

TB Register

Quarterly Report on theTreatment Outcome ofPulmonary TB Cases

* Cure rate:

Number of cases who were cured--------------------------------------------------------------- x 100

Total number of cases registered

* Completion rate:Number of cases who completed treatment

--------------------------------------------------------------- x 100 Total number of cases registered

* Death rate:

Number of cases who died during the treatment

--------------------------------------------------------------- x 100


*Failure rate:

Number of smear positive cases who still smear positive at fivemonths or more of treatment

-------------------------------------------------------------- x 100


* Defaulter rate:

Number of cases who defaulted

-------------------------------------------------------------- x 100


* Transfer-out rate:

Number of cases who transferred to another

DOTS facility with a proper referral / transfer slip

---------------------------------------------------------------- x 100


PPMD Units

8. Additionality Number of new smear-positive TB cases detected by PPMD*--------------------------------------------------------- x 100

Total number of new smear-positive TB cases detected bycity/municipality /province/PPMD

*Note: PPMD refers to cases either detected by a private-initiatedPPMD Unit or referred by a private physician to a public-initiated

PPMD Unit

TB Register

Overview of the Health Promotion Program for the NTP

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Health Promotion (HP) is the process of enabling people to take action to improve their health.

Guiding principles for the health promotion component of the National Tuberculosis Control Program

are anchored on the provisions of Administrative Order No. 58 issued by the National Center for Health

Promotion (NCHP) of the Department of Health. Under this set up, there are five general action areas

for health promotion: 1) building health public policy; 2) creating supportive environment; 3) developing

personal skills of the general public; 4) reorienting health services; and 5 strengthening community

participation.

1. Building Health Public Policy

HP goes beyond health care. It puts health on the agenda of policy makers in all sectors and

at all levels, directing them to be aware of the health consequences of their decisions and to accept

their responsibilities for health.

2. Creating Supportive Environment

The links between people and their environment constitute the basis for a socio-ecological

approach to health. Changing patterns of life, work, and leisure have a significant impact on health.

Work and leisure should be a source of health for people. HP generates living and working conditions

that are safe, stimulating, satisfying, and enjoyable.

3. Developing Personal Skills

HP supports personal and social development through information, education for health, and

enhancing life skills. By so doing, it increases the options available to people to exercise more

control over their own health and over their environments, and to make choices conducive to health.

4. Reorienting Health Services

The responsibility for HP in health services is shared among individuals, community groups,

health professionals, health service institutions, and government. They must work together towards

a health care system which contributes to the pursuit of health.

5. Strengthening Community Action

HP works through concrete and effective community action in setting priorities, making

decisions, planning strategies, and implementing them to achieve better health. At the heart of this

process is the empowerment of communities – their ownership and control of their own endeavors

and destinies.

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There are also different communication strategies for HP. These are advocacy, social

mobilization, health education, social marketing, community organizing, and counseling. These

and other strategies may be adopted to increase the intended stakeholders’ level of awareness

and to promote health-seeking behavior for early case detection and assurance of cure.

TB Network (“Kakampi Laban sa TB!” and “Sama-samang sugpuin ang TB!”) is the

official communication handle of the NTP. It also serves as the overarching brand for DOH’s re-

energized fight against TB as it forges partnerships between the public and the private sectors.

The key players in this partnership are DOH, Philippine Coalition Against Tuberculosis (PhilCAT),

Philippine Health Insurance Corporation (PHIC), Local Government Units (LGUs), and the various

DOTS facilities nationwide. During the commemoration of World TB Day (March 24) and National

TB Day (August 19) every year, partnerships and collaborations between and among the public

and private partners are strengthened and highlighted.

Documentation of testimonials and best practices for better HP outcomes are also

important for developing better strategies for HP and eventually better NTP accomplishments.

Any HP activity useful for expediting certification and accreditation of DOTS facilities and promoting

PPMD may also be considered.

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Table 7.1 presents the five areas of health promotion and the corresponding main tasks, intended

audiences, and strategies/major activities. The suggested key messages for each area are also given.

Table 7.1. Health Promotion Activities for Addressing Various Tasks

Areas of HealthPromotion

Main Tasks IntendedAudiences/

Stakeholders

Strategies/MajorActivities

Suggested KeyMessages

1. Buildinghealth publicpolicies

General politicalsupport(financial,issuance ofordinances/resolutions)

LegislatorsDonor agenciesLocal ChiefExecutives

AdvocacySocial marketingLobbyingSensitization

“TB control is anational priority.”“TB is a major publichealth problem.”“ TB is the 6th leadingcause of illness anddeaths in thePhilippines.”“TB affects the mosteconomicallyproductive age-groupresulting in enormouseconomic losses.”“DOTS is the mostcost- effective strategyto control TB.”

2. Creatingsupportiveenvironment

Generate multi-sectorial support

GOsNGOsProfessionalsocietiesBusiness sectorAcademeMedia

Social mobilizationNetworkingAdvocacy Alliancebuilding/localcoalition buildingTB Networkcommemoration ofinternational andnational TB eventsEnsuring availabilityof services, drugs,supplies, etc. CUPdissemination IEC(Airing of DOTSjingle)

“TB is everyone’’sconcern.”“TB is a major publichealth problem”“Forging partnershipsand collaborations inall sectors is the keyto TB control.”

3. Developingpersonal skills

Improve healthseekingbehavior (forearly casedetection andassurance ofcure)

TBSymptomaticsTB patientsGeneral public

Social marketingHealth educationPatient educationCounselingIEC (Media campaign:radio, TV, print,cinemas, internet)Enter-educateactivities KAP Surveys(Pre-Post

“TB is everyone’sconcern”“TB kills.”“TB is infectious butcurable.”“DOTS services areavailable for freenationwide.”

Household healthteachingsParent’s classes/Testimonials

TEN COMMANDMENTS FOR TB ADVOCATES

1. Advocates have a duty to respect the dignity, privacy, and self-determination of the clientele.

2. Advocates have a duty to treat everyone they encounter in their work fairly, honestly, and with

respect.

3. Advocates shall endeavor to develop partnerships with present and past recipients of DOTS

services to involve them directly in advocacy activities and to enrich advocacy efforts.

4. Advocates have a duty to be responsive to clients’ complaints and recommendations concerning

the provision of advocacy services.

5. Advocates have a duty to identify, avoid actual and potential conflicts of interest which may

compromise their ability to represent and safeguard the rights of the target beneficiaries.

6. Advocates must seek to assist their clients to participate in making decisions about advocacy

activities and in advocating on their behalf.

7. Advocates must assure that their clients are fully informed about advocacy activities undertaken,

about information which is gathered in the course of advocacy, and about reasonable courses of

actions, implications of actions, and potential outcomes.

8. Advocates have a duty to present facts accurately and honestly.

9. Advocates have a duty to understand applicable laws and procedures for enforcing it.

10. Advocates have a duty to know and improve their own skills and knowledge

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4. Reorientinghealthservices

Encourage &sustain healthproviders’participation inquality DOTSimplementation

All health workers(public andprivate)

Capability-buildingtrainings, refreshercourses,orientation/salesconferences)Recognitions (MLQAwards)Formative research/Monitoring andEvaluationDocumentation

“TB Control is anational priority.”“DOTS is the strategyto control TB.”“DOTS ensures cure.”“DOT with a treatmentpartner ensures cure.”

5. Strengtheningcommunity action

EncouragecommunityparticipationEmpowercommunity

Localofficials/LeadersPeople’sOrganizationsCivic groupsInformal sectorsCommunitygroups

Communityorganizing, Primaryhealth care,Organization ofsupport groups (TBTask Forces/ TBpatients Advocates),Communityassemblies,Household healthteachings,Parents’ clases,Testimonials,Recognition/Awards

“If you have cough fortwo weeks or longer,you may have TB.”“Consult at the nearestDOTS facility if youhave symptoms ofTB.”“DOTS services areavailable for freenationwide”“TB is curable”“TB affects everyone.”“Daily intake of anti-TB drugs ensurescure.”“DOT with a treatmentpartner ensures cure.”

Annex 1

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The TB Diagnostic Committee (TBDC)

BACKGROUND AND RATIONALE

The DOTS Strategy was pilot-tested in the Philippines’ NTP in 1996, and was subsequently

expanded throughout the country. However, the smear (+) cases represented only about 35 percent of

the pulmonary TB cases;1 among the smear-negative but X-ray positive TB cases, about 30-50 percent

were thought to be inactive TB cases. Most of these cases were referrals from the private sector.

A 1997 study conducted in the NTP DOTS pilot sites showed that among cases diagnosed by

chest X-ray, only 25 percent had radiographic findings suggestive of active PTB, 36 percent had “suspicious

shadows” only (or doubtful TB activity), and 39 percent had either normal X-rays or radiographic lesions

secondary to other diseases (Chaulet, P; WHO). There was a high level of over-reading and over-

diagnosis that led to the unnecessary anti-TB treatment of many patients. These patients were subjected

to the psychological burden of being labeled as TB patients, and were exposed to the potential adverse

effects of the anti-TB drugs. Moreover, the situation resulted in the waste of limited resources, particularly

anti-TB drugs.

These observations demonstrate the inherent problems, and the relatively low accuracy, of the

X-ray based diagnosis of TB. To improve the quality of diagnosis among the smear- negative/X-ray

positive TB suspects in DOTS areas, the NTP created TB Diagnostic Committees (TBDC) at the provincial

or city level. These committees were tasked to evaluate the clinical data and X-ray films of the smear-

negative/X-ray positive TB suspects, and to come up with the diagnosis and corresponding therapeutic

recommendations (by consensus) for these patients. The TBDC was subsequently integrated into the

NTP framework for TB case finding.

1 Ahn, DI. Mission Report; TB Prevention and Control. World Health Organization. 1998.

Annex 3

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OBJECTIVES

General Objective

TBDC was created to improve the quality of diagnosis among smear-negative PTB cases.

Specific objectives

1. Reduce the level of over-diagnosis and over-treatment among smear-negative PTB cases.

2. Ensure that active cases of smear-negative PTB are detected, and are provided with the appropriate

anti-TB treatment.

TBDC COMPOSITION AND ROLES OF COMMITTEE MEMBERS

The TBDC is chaired by the public sector (NTP Medical Coordinator) whose members come

from the public and the private sectors representing various disciplines. The TBDC is established at the

province or city level, or as an added option, at the district level. The composition of the TBDC is as

follows:

Provincial/City TB Diagnostic Committee:

1. Provincial/City NTP Medical Coordinator

1.1 Acts as the Chairperson of the TBDC (Note: Another TBDC member may be designated as

co-chairperson.)

1.2 Organizes the Committee

1.3 Convenes the Committee regularly

1.4 Moderates the discussions of the committee

1.5 Prepares the quarterly reports of the TBDC

1.6 Monitors and supervises the outputs of the TBDC activities

2. Radiologist

2.1 Reviews, together with the other Committee members, the referred X-ray films

2.2 Provides a description and interpretation of the X-ray findings that will serve as one of the

bases for diagnosis and treatment

3. Clinician/Internist/Pulmonologist

3.1 Provides an analysis of the clinical data of each case for correlation with the radiographic

findings

3.2 Recommends the appropriate intervention(s) for the referred patients

4. Provincial/City NTP Nurse Coordinator

4.1 Consolidates the necessary documents of referred cases prior to each meeting

4.2 Acts as the Committee Secretariat

4.3 Monitors and supervises the outputs of the TBDC activities under the direction of the Chairperson

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ORGANIZING THE TB DIAGNOSTIC COMMITTEE

1. The NTP Coordinators (Provincial or City level) will initiate a preliminary meeting/discussion with

the PHO/CHO regarding the prospective members of the Committee.

2. An initial meeting with the potential members will be convened by the Province/City NTP Coordinators,

in consultation with the PHO/CHO, to discuss the creation of the Committee. The CHD NTP

Coordinators may be invited to provide technical inputs. The participants will be given an orientation

on the NTP, and on the TBDC.

3. The solicitation of membership will be formalized by the PHO/CHO. The operating details, such as

the venue and schedule of the TBDC sessions, will also be finalized.

4. A copy of the final list of members will be provided to the Provincial/City health office and CHD.

Note: A district level TB Diagnostic Committee may also be established as an option, to make the TBDC services more accessible to the peripheral

health units and to reduce the volume of referrals to the Provincial TBDC. The district level TBDC reports to the Provincial/City Medical coordinator.

Monitoring of the district TBDC is the responsibility of the Provincial/City NTP coordinators.

RECORDING AND REPORTING

The TBDC shall make use of the prescribed TBDC referral, recording, and reporting forms (see Chapter

IV – Recording and Reporting). The quarterly TBDC report shall be prepared by the NTP coordinators and submitted

to the CHD together with the other NTP quarterly reports.

FORM GENERAL DESCRIPTION RESPONSIBLEPERSON

TBDC Referral Form Used for referring smear- negative TB suspects to theTBDC. The form has two parts:

Upper portion contains general information about thepatient.

Lower portion contains the TBDC findings/decisionsand recommendations.

Upper portion to be filled-up by the Physician orNurse of the referringDOTS facilities

Lower portion to be filled-up by the TBDCSecretariat, duly signed bythe TBDC Chairpersonand Secretariat

TBDC Masterlist This is the listing of all smear- negative TB suspectsreferred to the TBDC.

TBDC Secretariat

This is the accomplishment report of the TBDCsubmitted to the CHD on a quarterly basis.

Provincial /City Medicalor Nurse NTPCoordinators

Quarterly TBDCReport Form

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TB DIAGNOSTIC COMMITTEE OPERATING PROCEDURES

1. The Secretariat consolidates all documents (including X-ray films) pertaining to each referred case

on the TBDC Masterlist.

2. The Committee reviews/correlates all the documents and deliberates on each referred case during

its regular sessions.

The Committee arrives at a consensus regarding the diagnosis and recommendations on patient

management based on the recommended Diagnostic Flowchart (Flow chart for the diagnosis of

smear-negative pulmonary TB). If the Committee feels the need to see the patient, then the patient

will be invited on the next Committee session.

4. The Secretariat writes the TBDC diagnosis and recommendations on the lower portion of the TBDC

Referral Form in accordance with the discussions during the TBDC session. Both the Chairperson

and the Secretariat should affix their signatures on the completed form.

5. The completed TBDC Referral Form is sent back to the referring DOTS facilities for implementation

of the TBDC recommendations. For patients who are recommended for anti-TB treatment, their

respective TBDC Referral Forms should be attached to their respective NTP Treatment Cards. All

other completed TBDC referral forms should be filed for future reference.

TBDC sessions shall be held at least twice a month.

MONITORING AND EVALUATION

Monitoring and evaluation of the TBDC shall be done in conjunction with the regular NTP

monitoring and program review. The NTP Staff of the NCDPC and other TB partners can join the CHD

in the monitoring and evaluation of the TBDC. The TBDC Chairperson shall also ensure that these

recommendations are implemented by the DOTS facilities accordingly.

REFERRAL PROCEDURES (Referring Unit Level)

The DOTS facilities shall refer to the TBDC all smear-negative/X-ray positive TB suspects using

the TBDC Referral Form. The referring unit’s physician or nurse shall fill up completely the upper

portion of the TBDC Referral Form.

The referring unit should follow the “Flowchart for the Diagnosis of Smear- Negative PTB” (see

Figure 2.2. Flow chart for the diagnosis of smear-negative pulmonary TB).

3. The referring unit sale ensure that all the available chest X-ray films (including old films) and properly

filled up TBDC Referral Form of each referred patient are submitted to TBDC.

3.

6.

2.

1.

procedure man tb

Documents

bold capital

medicos del

periodic independent

proper referral

ntp id cards

creating supportive

exceptional

primary diagnostic