Antifungals 101

1. Antifungals 101 Dr. HeshamAmgad Senior ICU phamacist / DIC pharmacist CCHE

2. I. AZOLES • Members of the triazole family are some of the most widely used antifungal agents. • Inhibit Ergosterol synthesis (important component of fungal cell membranes). • Fungistaticagainst Candida species. • Voriconazole fungicidal activity against Aspergillusspecies. • Main metabolism is hepatic, main toxicity is elevated LFTs. • Major drug-drug interactions.

3. A. FLUCONAZOLE • Drug of choice for non-severe Candida infections, including C.albicans, except C.glabrata (can overcome with higher doses) and C.krusei (completely resistant) • Also used for Cryptococcus infections (maintenance phase for cryptococcal meningitis after induction with Ampho B), Coccidioidomycosis, Histoplasmosis, and others. • Toxicity: elevated LFTs, also GI side effects. • Great CSF and urine penetration (only azole with good urine penetration). •  Available in both oral and intravenous preparations.

4. B. VORICONAZOLE • Cidal for many molds, drug of choice for Invasive Aspergillosis. • Also effective against most Candida, but little reason to use over Fluconazole. • One important hole in coverage is no Zygomycetes (Mucormycosis) • Liver toxicity, also visual toxicity; transient visual changes, but also rare visual hallucinations. •  Available in both oral and intravenous preparations. • Oral bioavailability is reduced by approximately 30% when taken with a high fat meal; must be taken on empty stomach. • Intravenous formulation contains cyclodextrin vehicle which is nephrotoxic. • Good CSF penetration.

5. C. ITRACONAZOLE • Used for non-severe Histoplasmosis and Blastomycosis. • Toxicity: LFTs and also negative inotrope, can worsen or cause CHF in predisposed patients, GIT side effects with solution form. • Available as a capsule, and an oral solution. • Capsule formulation has a bioavailability of approximately 55%, solution is 30% more. • Capsules require food and an acidic gastric pH for solubilization. • Bioavailability of oral solution is not altered by gastric pH; should be administered on an empty stomach for optimal absorption.

6. D. POSACONAZOLE • Newest Azole with broad spectrum of activity; yeast, molds, endemic fungi, Zygomycetes (only azole with activity). • Used as 2nd-line / salvage therapy for many severe fungal infections. • Main problem is that it is only available PO, and must be given with fatty foods for maximal absorption.

7. II. AMPHOTERECIN B • Polyene , binds ergosterol in membrane and forms membrane pores. • Drug of choice for many severe fungal infections: Zygomycetes, Cryptococcal Meningitis (induction phase with flucytosine), Severe Histoplasmosis/Blastomycosis/Coccidioidomycosis. • 2nd-line for invasive aspergillosis (Voriconazole is DOC) • 2nd-line for candida infections (Echinocandins are at least as effective, and less toxic) • Some candida are resistant. • Significant toxicity: Nephrotoxic (including Mg and K wasting), hypotension, bradycardia, fevers/chills during infusion, seizures. • ABELCET (lipid complex), AMBISOME (liposomal): Lipid preparations that are equally effective and much less toxic (esp. renal toxicity), although more expensive. • Allow for much higher doses thanks to lower toxicity. • Only lipid preparations have good CSF penetration.

8. III. ECHINOCANDINS • New class of antifungals;inhibit beta-(1,3)-D-glucansynthase, an enzyme that is necessary for the synthesis of an essential component of the cell wall of several fungi. • Caspofungin, Micafungin, and Anidulafungin. • All three echinocandins share a similar spectrum of activity, but differ in dosing, pathways of metabolic elimination, and drug interaction profile. • Lower incidence of side effects and drug interactions compared to other antifungals. • Drug of choice for candida infections especially in critically ill and neutropenic patients. • Salvage therapy for Invasive Aspergillosis. • Low CNS penetration. • Toxicity: elevated LFTs, GIT.

9. Thank You