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Effects of Liver Disease on Pharmacokinetics Juan J.L. Lertora, M.D., Ph.D. Director Clinical Pharmacology Program October 29, 2015 National Institutes of Health Clinical Center

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Page 1: Effects of Liver Disease on Pharmacokinetics of Hepatic Clearance - Effect of Liver Disease on Elimination: - ... The same diagram now including volume and concentration terms and

Effects of Liver Disease on Pharmacokinetics Juan J.L. Lertora, M.D., Ph.D.

Director Clinical Pharmacology Program

October 29, 2015 National Institutes of Health

Clinical Center

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2

GOALS of Liver Disease Effects Lecture -Estimation of Hepatic Clearance

- Effect of Liver Disease on Elimination:

- RESTRICTIVELY Eliminated Drugs

- NON-RESTRICTIVELY Eliminated Drugs

- Other Effects of Liver Disease:

- Renal Function

- Drug Distribution

- Drug Response

- Modification of Drug Therapy in Patients with Liver Disease

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3

Correlation of Lab Test Results with Impaired CYP Enzyme

Function

The Central Problem

There is no laboratory test of liver function that is as useful for guiding drug dose

adjustment in patients with liver disease as is the estimation of creatinine clearance in

patients with impaired renal function.

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4

FDA Approved Drug Labels Dosing Guidance in Liver Disease

Evaluation of hepatic impairment dosing recommendation in FDA approved product

labels.

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5

ADDITIVITY of Clearances

Equation showing that total elimination clearance equals the sum

of renal and nonrenal clearances

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6

CALCULATION OF CLH

Equation showing that hepatic clearance is estimated as the total clearance minus the

renal clearance, assuming that it equals non-renal clearance.

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7

FICK EQUATION

Defines clearance as liver blood flow times the extraction ratio A-V/A.

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8

Derivation of Rowland Equation (I)

Diagram of hepatic capillary blood flow, fraction of unbound drug and intrinsic clearance

with the “well-stirred” model.

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Derivation of Rowland Equation (II)

The same diagram now including volume and concentration terms and a mass balance

equation for hepatic drug clearance.

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10

Derivation of Rowland Equation (III)

The same diagram with a derivation of an extraction ratio term that includes unbound

fraction, intrinsic clearance, and liver blood flow.

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11

Rowland Equation WELL-STIRRED COMPARTMENT

Rowland Equation for hepatic clearance.

Two limiting cases:

Restrictively metabolized drugs (influenced by protein binding)

Non-restrictively metabolized drugs (blood flow-dependent)

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RESTRICTIVELY AND NON-RESTRICTIVELY

ELIMINATED DRUGS

RESTRICTIVELY METABOLIZED DRUGS:

Phenytoin

Warfarin

Theophylline

NON-RESTRICTIVELY METABOLIZED DRUGS:

Lidocaine

Propranolol

Morphine

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13

HEPATIC FIRST-PASS METABOLISM

Equation for the extraction ratio A-V/A.

Illustration of hepatic first-pass metabolism and the portal and systemic circulations.

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NON-RESTRICTIVELY Eliminated Drugs

These drugs have extensive first-pass metabolism.

Equation showing that hepatic clearance is a function of liver blood flow.

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15

ACUTE VIRAL HEPATITIS - Acute inflammatory condition

- Mild and transient changes related to extent of disease in most cases. Infrequently severe and fulminant

-May become chronic and severe

- Changes in drug disposition less than in chronic disease

- Hepatic elimination returns to normal as disease resolves

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CHRONIC LIVER DISEASE - Usually related to chronic alcohol use or viral hepatitis - Irreversible hepatocyte damage

─ Decrease in SERUM ALBUMIN concentration

─ Decrease in INTRINSIC CLEARANCE of drugs

─ Intrahepatic and extrahepatic shunting of blood from

functioning hepatocytes

─ FIBROSIS disrupts normal hepatic architecture

─ NODULES of regenerated hepatocytes form

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17

RESTRICTIVELY METABOLIZED DRUGS: EFFECTS OF

LIVER DISEASE Equation showing that hepatic clearance equals unbound fraction times the

intrinsic clearance.

Chart showing that hepatic clearance increases if albumin decreases, and decreases if

intrinsic clearance decreases.

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18

RESTRICTIVELY METABOLIZED DRUGS:

EFFECT OF PROTEIN BINDING CHANGES

Equations showing that free drug concentration at steady-state is a function of dosing rate

and intrinsic hepatic clearance.

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19

FREE and TOTAL PHENYTOIN Levels

(DOSE = 300 MG/DAY)

Chart showing that total Phenytoin concentration is lower than normal in functionally

anephric patients but free Phenytoin concentration is the same.

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20

RESTRICTIVELY METABOLIZED DRUGS: EFFECT

OF PROTEIN BINDING CHANGES

Chart showing a protein binding interaction with Warfarin. There is a transient increase

in free Warfarin concentration and prothrombin time.

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21

RESTRICTIVELY METABOLIZED DRUGS: EFFECTS OF LIVER DISEASE

Equation showing that hepatic clearance equals unbound fraction times the

intrinsic clearance.

Chart showing that hepatic clearance increases if albumin decreases, and decreases if

intrinsic clearance decreases.

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22

ROLE OF CYP ENZYMES IN HEPATIC DRUG

METABOLISM

Pie chart showing relative hepatic content of CYP enzymes and pie chart showing % of

drugs metabolized by CYP enzymes.

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RESTRICTIVELY METABOLIZED DRUGS: EFFECT

OF CIRRHOSIS ON Clint

Chart illustrating % of normal intrinsic clearance for normal, mild, moderate, and severe

cirrhosis, and the impact on glucuronidation and CYP2D6, CY3A4, CYP2C19, and

CYP1A2.

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PUGH-CHILD CLASSIFICATION OF LIVER DISEASE SEVERITY

Chart showing assessment parameters and assigned scores in addition to classification of

clinical severity of mild, moderate and severe.

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CORRELATION OF SPECIAL TESTS OF LIVER FUNCTION

WITH CHILD-PUGH SCORES*

Chart showing changes in indocyanine green and sorbitol clearances, and the galactose

elimination and the antipyrine breath tests.

* Data from Herold C, et al. Liver 2001;21:260-5.

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“PITTSBURGH COCKTAIL” APPROACH

DRUG ENZYME

CAFFEINE CYP 1A2

CHLORZOXAZONE CYP 2E1

DAPSONE CYP 3A + NAT2

DEBRISOQUIN CYP 2D6

MEPHENYTOIN CYP 2C19

* From: Frye RF, et al. Clin Pharmacol Ther 1997;62:365-76

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RESTRICTIVELY METABOLIZED DRUGS:

EFFECTS OF LIVER DISEASE

Equation showing that hepatic blood flow equals unbound fraction times the

intrinsic clearance.

Chart showing that hepatic clearance increases if albumin decreases, and decreases if

intrinsic clearance decreases.

Portosystemic shunting reduces total hepatic clearance and increases free drug

concentration.

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28

EFFECTS OF HEPATIC SHUNTING ON ROWLAND EQUATION*

Modified Rowland Equation accounting for shunt blood flow.

* From: McLean A, et al. Clin Pharmacol Ther 1979;25:161-6.

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RESTRICTIVELY METABOLIZED DRUGS: EFFECTS OF HEPATIC SHUNTING*

Chart showing liver disease severity, QT, QP, QP/QT, and Antipyrine CLH

*From: McLean A, et al. Clin Pharmacol Ther 1979;25:161-6.

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30

NON-RESTRICTIVELY METABOLIZED DRUGS: EFFECTS OF LIVER DISEASE

Equation for hepatic clearance = blood flow showing that changes in protein binding and

intrinsic clearance have no impact on hepatic clearance for these drugs.

Chart

* However, note that free concentration is

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31

NON-RESTRICTIVELY METABOLIZED DRUGS: EFFECTS OF LIVER DISEASE

Equation for CLH =Q

Equation for hepatic clearance = blood flow showing that changes in protein binding and

intrinsic clearance have no impact on hepatic clearance for these drugs.

HOWEVER, fuCLint MAY NO LONGER BE >> Q

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NON-RESTRICTIVELY METABOLIZED DRUGS: EFFECTS OF LIVER DISEASE

Equation for CLH = Q

Equation for hepatic clearance = blood flow showing that changes in protein binding and

intrinsic clearance have no impact on hepatic clearance for these drugs.

Decreased hepatic perfusion results in increased oral bioavailability (F).

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EFFECTS OF HEPATIC SHUNTING ON ROWLAND EQUATION*

Modified Rowland Equation

* From: McLean A, et al. Clin Pharmacol Ther 1979;25:161-6.

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NON-RESTRICTIVELY METABOLIZED DRUGS: EFFECTS OF DECREASED

LIVER PERFUSION*

Chart showing liver disease Severity, QT, QP, QP/QT, and ICG CLH (clearance of

indocyanine green)

* From: McLean A, et al. Clin Pharmacol Ther 1979;25:161-6.

Page 35: Effects of Liver Disease on Pharmacokinetics of Hepatic Clearance - Effect of Liver Disease on Elimination: - ... The same diagram now including volume and concentration terms and

35

INFLUENCE OF PORTOSYSTEMIC SHUNTING

ON ORAL BIOAVAILABILITY (f)

RESTRICTIVELY Eliminated Drugs:

Little change

NON-RESTRICTIVELY Eliminated Drugs:

SHUNTING may markedly increase oral bioavailability due to reduced first

pass metabolism drug bypasses hepatocytes

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36

CIRRHOSIS AFFECTS EXPOSURE TO SOME

NON-RESTRICTIVELY METABOLIZED DRUGS

Chart showing increased Absolute Bioavailability and relative exposure cirrhotics/control

of Meperidine, Pentazocine, and Propranolol.

* THIS ALSO INCORPORATES 55% INCREASE IN PROPRANOLOL fu

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37

CIRRHOSIS AFFECTS RENAL FUNCTION:

THE HEPATORENAL SYNDROME

-Risk in Patients with Cirrhosis, Ascitis, and GFR > 50

mL/min:

- 18% within 1 year

- 39% within 5 years

- Predictors of Risk:

- Small liver

- Low serum albumin

- High plasma renin

- Cockcroft and Gault Equation may overestimate

renal function

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38

CIRRHOSIS AFFECTS RENAL FUNCTION:

THE HEPATORENAL SYNDROME

- The Syndrome has a FUNCTIONAL

rather than an Anatomical Basis.

Page 39: Effects of Liver Disease on Pharmacokinetics of Hepatic Clearance - Effect of Liver Disease on Elimination: - ... The same diagram now including volume and concentration terms and

39

HEPATORENAL SYNDROME

ANTEMORTEM ARTERIOGRAM

There is no renal perfusion.

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40

HEPATORENAL SYNDROME

POSTMORTEM Arteriogram

Renal perfusion appears normal.

Page 41: Effects of Liver Disease on Pharmacokinetics of Hepatic Clearance - Effect of Liver Disease on Elimination: - ... The same diagram now including volume and concentration terms and

41

CIRRHOSIS AFFECTS RENAL FUNCTION: THE HEPATORENAL SYNDROME

- Therapy with some drugs may precipitate

Hepatorenal Syndrome

ACE Inhibitors

NSAIDs

Furosemide (High Total Doses)

Page 42: Effects of Liver Disease on Pharmacokinetics of Hepatic Clearance - Effect of Liver Disease on Elimination: - ... The same diagram now including volume and concentration terms and

42

CIRROSIS MAY AFFECT

DRUG DISTRIBUTION

- Increased Free Concentration of

NON-RESTRICTIVELY Eliminated Drugs

(e.g. PROPRANOLOL)

- Increased Permeability of Blood:CNS Barrier

(e.g. CIMETIDINE)

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43

CIRRHOSIS AFFECTS DRUG DISTRIBUTION: INCREASED CNS PENETRATION OF CIMETIDINE*

Chart showing cimetidine CSF/serum ratio from normal to renal + liver disease to liver

disease

* From Schentag JJ, et al. Clin Pharmacol Ther 1981;29:737-43

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44

CIRRHOSIS MAY AFFECT PHARMACODYNAMICS

- Sedative response to BENZODIAZEPINES is exaggerated

- Response to LOOP DIURETICS is reduced

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Drugs CONTRAINDICATED in Patients with Severe Liver Disease

- May precipitate renal failure:

- NSAIDs

- ACE Inhibitors

- Predispose to bleeding:

- β-LACTAMS with N-Methylthiotetrazole Side Chain

(e.g. CEFOTETAN)

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46

Drug Requiring ≥ 50% Dose Reduction in Patients

with MODERATE CIRRHOSIS

CHANGE IN CIRRHOSIS

F CLE

ANALGESIC DRUGS

Morphine ↑ 213% ↓ 59%

Meperidine ↑ 94% ↓ 46%

Pentazocine ↑ 318% ↓ 50%

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47

Drugs Requiring ≥ 50% Dose Reduction in Patients

with MODERATE CIRRHOSIS

CHANGE IN CIRRHOSIS

F CLE

CARDIOVASC. DRUGS

Propafenone ↑ 257% ↓ 24%

Verapamil ↑ 136% ↓ 51%

Nifedipine ↑ 78% ↓ 60%

Losartan ↑ 100% ↓ 50%

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Drugs Requiring ≥ 50% Dose Reduction in Patients

with MODERATE CIRRHOSIS

CHANGE IN CIRRHOSIS

F CLE

OTHER DRUGS

Omeprazole ↑ 75% ↓ 89%

Tacrolimus ↑ 33% ↓ 72%

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49

PUGH-CHILD CLASSIFICATION

OF LIVER DISEASE SEVERITY

Chart showing assessment parameters with assigned score and classification of clinical

severity of mild, moderate and severe.

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50

RECOMMENDED EVALUATION OF

PHARMACOKINETICS IN LIVER DISEASE

PATIENTS*

REDUCED Study Design:

- Study Control Patients and Patients with Child-Pugh

- Moderate Impairment

- - Findings in Moderate Category Applied to Mild

- Category; Dosing Prohibited in Severe Category

FULL Study Design:

- Study Control Patients and Patients in All Child-Pugh

Categories

- Population PK Approach

* FDA Clinical Pharmacology Guidance, May 2003