janin on fungal infections

21
Fungal Infection s Dr P. Janin RNSH

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Pierre Janin is an intensivist with many interests. For example you may have seen his fantastic echo guide or his talk on transcranial doppler. One of his other passions is microbiology, and at BCC last year he gave this talk on Fungal infections. He often proudly shows pictures of his fungal balls on ward rounds.

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Page 1: Janin on Fungal Infections

Fungal Infections

Dr P. JaninRNSH

Page 2: Janin on Fungal Infections

Introduction

• Complex names, description, and classification

• Difficult diagnosis

• Difficult treatment strategy

Page 3: Janin on Fungal Infections

Importance

• More than 100 000 species• Small subset can cause human disease

• Increasing incidence• Disease of modern Medicine• Aspergillosis:

10 000 hospitalization /year (USA)20% increase compared with previous 2

decades.

• Mortality ~100% if left untreated.

• Substantial financial burden• Annual cost for candidemia: $44-320 million (USA)• Hospitalization for Aspergillosis: >$60 000

Page 4: Janin on Fungal Infections

Principles

• Subcutaneous, Cutaneous, Superficial mycosis

• Endemic mycoses• Histoplasma, Bastomyces, Coccidioides• Restricted to specific areas. Less relevant in Australia.• Wide variety of syndromes

• Opportunistic fungal infections• The most relevant category in ICU patients• Both yeasts and moulds• Associated with many difficulties

Page 5: Janin on Fungal Infections

Principles

• Many species are free living in the environment (moulds), or are part of the normal flora (candida)• Continuous exposure• Normally well controlled in immunocompetent host

• Many fungi are saprohytes• Disease when tissue becomes “inert”: profound

immunosuppression• Direct inoculation

• Diagnostic problem• Colonization vs Invasive infection

Page 6: Janin on Fungal Infections

Principles• Protagonists in ICU :

• Invasive Candidiasis• Represents over 10% of infections in ICU• Rates in the ICU >10-fold those on the wards• Probably underestimated

• Invasive Aspergillosis and other mould pathogens• Transplant patients, haematological conditions, immunosuppressed• Other patients (lung disease, liver failure). Uncommon.• Fusarium, Scedosporium, Zygomycetes

• Pneumocystis

• Cryptococcus

Page 7: Janin on Fungal Infections

Candidiasis

• Emergence :

• Normal colonizer of GI tract. Most infections are endogenous.

• GI tract surgery

• Immunosuppression, including :• Broad spectrum antibiotics• Neutropenia and Decreased T-cell immunity• Invasive devices (CVC, Dialysis, TPN)

• Extensive candidiasis develops early when integrity of natural barriers is compromised• Risk assessment

Page 8: Janin on Fungal Infections

• Culture from normally sterile sites, including blood cultures• Newer techniques not sufficiently validated

• High mortality rate (25-38% for candidemia, at least in part due to the infection itself)

• Many species• Different susceptibility profiles• No prediction model shown accurate

Candidiasis• Invasive Candidiasis :• May affect virtually every organ (micro-abscesses)• Vulnerable sites : endophtalmitis, meningitis, vertebral

osteomyelitis, hepatosplenic abscesses, endocarditis (prosthetic valves)

Page 9: Janin on Fungal Infections

Candidiasis• Echinocandin (Caspofungin, Anidulafungin,

Micafungin) as initial choice

• Many patients have prior Azole exposure. Selection of resistant organism• C. glabrata• C. krusei (intrinsic)

• Clinical superiority compared to Azoles?• Theoretical fungicidal benefit• Anidulafungin vs Fluconazole

C. Reboli & Al. – NEJM 2007;356:2472-2482Non inferiority trial

D. R. Andes & Al. - Clinical Infectious Disease 2012;54(8):1110-1122

Page 10: Janin on Fungal Infections

• Other considerations:

• Bypasses the problem of drug interactions

• Caspofungin: agent with extensive data in Neutropenic patients• Amphotericin B still preferred ?

• C. parapsilosis: higher MIC ; no outcome implication?

Candidiasis• Echinocandin (Caspofungin, Anidulafungin,

Micafungin) as initial choice

Page 11: Janin on Fungal Infections

Candidiasis• Echinocandin (Caspofungin, Anidulafungin, Micafungin) as initial

choice

• Other considerations:

• Only Fluconazole can achieve sufficient concentrations in urine• Problem of fungal balls

• Eye/CNS diffusion: Flucytosine, Fluconazole, Amphotericine B

• Hepatotoxicity …

• Removal of CVC: associated with decreased mortality

• Mortality benefit of early treatment implementation• Days rather than hours

Page 12: Janin on Fungal Infections

Candidiasis

• Combination therapy ?

• CNS infections

• Prosthesis (prosthetic joints, …)• Flucytosine better than Fluconazole on biofilms

• Endocarditis

Page 13: Janin on Fungal Infections

Moulds

• Diagnostic problem• Infect areas in direct contact with the environment• Culture and examination of superficial specimen : contaminants• Biopsy

• Treatment problem• Resistant organism• Empirical treatment: risk of inadequacy• Conservative treatment: often insufficient

• Aspergillus• Zygomycetes (Mucor, Rhizopus)• Other (Scedosporium, Fusarium)

Page 14: Janin on Fungal Infections

Aspergillus

• Haematology patients: 2 waves• Neutropenia• Post-acute phase: Steroids (GVHD)

• Epidemiology• Important data to identify patients at risk• Derives the required pre-test probability• Very difficult

• By far the most common opportunistic mould• Invasive pulmonary Aspergillosis• Aspergilloma

Page 15: Janin on Fungal Infections

Aspergillus

• Diagnostic issues• Halo sign only if neutropenic• Sputum production is minimal if neutropenic• Poor performance of testing

• Limitations of empirical approach• Selection of rare pathogens (underlying condition, antifungal

prophylaxis)• No satisfying broad empirical coverage• Interfere with future diagnostic attempts

• Strategy• Empirical approach• Diagnostic approach• No very satisfying guideline

Page 16: Janin on Fungal Infections

Pre-disease Tests

• ß-D-Glucan• Attempt to solve issue of slow growth of Candida from BC• False positive common. Moderate performance (PPV ~55%).• May exclude Pneumocystis if negative?

• Galactomannan• Proposed as screening test for high risk patients• Interference with ß-Lactams (Tazocin), and fungal prophylaxis• Non reproducible results on Australian samples• Role when used on BAL samples ?

• Highly standardized technique (120mL, Centrifugation)• Cut-off? 1.0?

• Good negative predictive value

• Serologic tests• ß-D-Glucan: fungus (non Cryptococcus,

Zygomycetes)• Galactomannan: Aspergillus• PCR: not validated

Page 17: Janin on Fungal Infections

Anti-fungals• Difficult use• Spectrum inadequate for empirical use• Which end-points? (fever not reliable, …)• Side effects• Drug interactions• Pharmacodynamics/Pharmacokinetics

• Diffusion problem• Dose adjustment

• 3 major classes• Triazoles

• Fluconazole, Itraconazole, Voriconazole, Posaconazole• Echinocandins

• Caspofungin, Anidulafungin, Micafungin• Amphotericin B• Flucytosine

Page 18: Janin on Fungal Infections

Fluconazole• Linear pharmacokinetics. Predictable levels.• Loading dose

• Tubular reabsorption• Increased clearance in CVVH

• Non optimized dosing accounts for treatment failure ?

Page 19: Janin on Fungal Infections

Other Triazoles• Itraconazole• Concominant use of PPI: major impingement on absorption• Cyclodextrine

• Increased absorption• Increased nausea/diarrhea• Accumulation in renal failure

• Voriconazole• Complex pharmacokinetics• No impact of PPI• Large individual variations (CYP2C19):

• Poor (Chinese) vs high metabolizers• Highly variable concentrations

• Very often under-dosed• 4 mg/Kg q12h, after loading dose• Saturable excretion: risk of overdosing!

• Interactions: Phenytoin, Rifampicin, Corticosteroids

Page 20: Janin on Fungal Infections

Other Triazoles

• Posaconazole• IV formulation available in the future• Interference by PPI, mucositis, fatty meal• Limited benefit in acute setting

• 100h for steady state

Page 21: Janin on Fungal Infections

Conclusion• An expanding problem of modern medicine• Vulnerable host• predisposing holes in the normal barrier• Holes in the prophylactic “immune system replacement therapy”

• True impact on outcome• more than just the effect of the underlying advanced disease

• Difficult diagnosis. Host is predisposed to a wide array of injuries.• Value of tissue / deep specimen collection

• Inconvenient empirical treatment• Difficult drugs. Difficult endpoints.• Role of TDM