AntiFungal Therapy - Zheng 5/12/16

Question 1

fungal infections

• superficial
• subcutaneous
• systemic

Answer 1

superficial: skin, hair, nails

subcut: dermis, subcutaneous tissues and/or adj structures

systemic: disseminated infection of internal organs

• HIV pts
• autoimmune pts
• cancer pts
• organ transplant pts
• widespread use of antibiotics

Question 2

antifungal drug classification

• location
• mech of action

Answer 2

location

1. systemic (oral and IV)
2. systemic (for mucocutaneous inf)
3. topical drugs

mechanisms/targets

1. nucleic acid synthesis inhibitor : flucytosine
2. cell wall disruptors : echinocandins
3. cell membrane disruptors (fungal cell membranes contain ergosterol instead of cholesterol)

• amphotericin B (amphipathic pore former)
• azoles (block ergo biosynth; gen toxic byproducts)
• nystatin (ergosterol binder; pore former)
• allylamines (block ergo biosynth; gen toxic byproducts)

Question 3

drugs for systemic infections

amphotericin B

• structure
• mech of action
• target fungi
• resistance
• clinical use

Answer 3

macrolide with amphipathic ring structure

mechanism of action:

• nonpolar side binds tightly to ergosterol in membrane
• polar side forms pores for ion leakage
  
  • mycosamine sugar is the key linker between amphotericin-ergosterol

**selective for ergosterol in fungal membrane (won’t hit human/bacterial cell membranes!)

targets

• yeast: Candida albicans, Cryptococcus neoformans
• endemic fungi: Blastomyces dermatitidis, Histoplasma capsulatum, Coccidioides immitus
• pathogenic molds: Aspergillus fumigatus, Mucor

resistance

• intrinsic resistance: Candida lusitaniae, Pseudallescheria boydii
• acquired resistance can occur in vitro via decreased/modified ergosterol or inability to penetrate cell wall BUT not clinically significant

clinical use

• drug of choice for life-threatening systemic inf BUT toxic side effects
  
  • often initial tx, followed by chronic tx with triazoles
• topical eyedrops for mycotic corneal ulcer/keratitis
• local injectction for fungal arthritis

Question 4

drugs for systemic infections

amphotericin B

• targets
• resistance
• clinical use

Answer 4

targets

• yeast: Candida albicans, Cryptococcus neoformans
• endemic fungi: Blastomyces dermatitidis, Histoplasma capsulatum, Coccidioides immitus
• pathogenic molds: Aspergillus fumigatus, Mucor

resistance

• intrinsic resistance: Candida lusitaniae, Pseudallescheria boydii
• acquired resistance can occur in vitro via decreased/modified ergosterol or inability to penetrate cell wall BUT not clinically significant

clinical use

• drug of choice for life-threatening systemic inf BUT toxic side effects
  
  • often initial tx, followed by chronic tx with triazoles
• topical eyedrops for mycotic corneal ulcer/keratitis
• local injectction for fungal arthritis

Question 5

drugs for systemic infections

amphotericin B

• admin
• PK
• toxicity

Answer 5

adminstration

• nearly insoluble in water
• not well absorbed orally → only given orally for GI inf
• given IV (suspension in deoxycholate)
• excretion: urine (halflife 15d)
  
  • levels not affected much by hepato/renal issues

**liposomal prep : lets you get higher doses with lower nephrotox BUT more expensive

toxicities

1. infusion related toxicity

• fever, chills, headache, vomiting, hypotension
• deal with it by…
  
  • decreasing dose
  • premed with antipyretics, antihists, meperidine, hydrocortisone

2. slower tox

• renal damage
• variable anemia
• occasional hepatic damage

drug interactions with nephrotoxic drugs (aminoglycosides, cyclosporine)

Question 6

drugs for systemic infections

flucytosine

• mechanism
• selectivity
• resistance

Answer 6

prodrug → eventually converted into nucleotide analogues that stall n.a. synth

mechanism of action

• taken up by fungal cytosine permease
• flucytosine → 5-fluorouracil [cytosine deaminase]
  
  • 5FU → 5FUTP : inhibits RNA synth
  • 5FU → 5FdUMP : inhibits DNA synth

selectivity

• cytosine permease only found in fungal cells - reason why this is a good antifungal but a lousy anticancer drug
• mammalian cells do not convert 5FC → 5FU well

resistance

• loss of 5FC → 5FU conversion
• loss of 5FU → 5FUMP conversion
• loss of cytosine permease

Question 7

drugs for systemic infections

flucytosine

• admin
• clinical use

Answer 7

oral administration → rapid absorption from GI

• distributes well (incl CSF)

removed by kidney (halflife 3-6hr)

• kidney dysfx → toxicity!

synergistic with amphoB, itraconazole

clinical use

• limited spectrum action : Candida, Cryptococcus
• typically given in combo to avoid resistance (with azoles, amphoB)

Question 8

drugs for systemic infections

flucytosine

• toxicity
• drug interaction

Answer 8

toxicity

• decrease fx of bone marrow (leukopenia, thrombocytopenia)
• rash, GI effects

why? conversion to 5FU by GI tract bacteria!

drug interactions with drugs that suppress bone marrow

Question 9

drugs for systemic infections

azoles

• classification

Answer 9

imidazoles (2N in 5 member ring)

• ketoconazole
• clotrimazole
• miconazole

triazoles (3N in 5 member ring)

• itraconazole
• fluconazole
• voriconazole

Question 10

drugs for systemic infections

azoles

• mech of action
• resistance

Answer 10

block P450 lanosterol demethylase (ERG11) → block ergosterol synthesis (3rd step)

• binds to active site
• diverts synth pathway to accumulation of toxic methylsterols → inhibit fungal enzymes localized on membrane

resistance

• pumps (similar to bacteria)
• alteration or overexpression of target : alters drug affinity
• ERG3 loss of fx : mitigation of toxicity

Question 11

drugs for systemic infections

azoles

• selectivity
• target
• toxicity
• drug interactions

Answer 11

selectivity

binds less effectively to mammalian P450s → somewhat specific for fungal cells

• Candida spp, Cryptococcus neoformans, endemic mycoses, dermatophytes, Aspergillus, Pseudallescheria boydii (amphoB resistant strain!)

toxicity

• minor GI distress
• liver enzyme abnormality → rare drug-induced hepatotox

drug int

• affects P450 drug metabolism (cyclosporine, warfarin, dihydropyridine, buspirone)

Question 12

imidazoles

Answer 12

ketoconazole

• first oral azole
• mostly replaced by triazoles, BUT is much cheaper

miconazole, clotrimazole

• only used topically

Question 13

triazoles

itraconazole

Answer 13

most potent azole → used for severe inf

favored over ketoconazole due to…

• broader spectrum
• fewer side effects (more selective)

administration/distribution/availability/metabolism

• oral admin (abs is improved with food/gastric acid)
• widely distributed, incl CSF
  
  • limited bioavailability → improved with cyclodextrin formulation
  • lipid soluble
• metabolized by liver via CYP 3A4 (halflife 30-40h)
  
  • primary metabolite (hydroxyitraconazole) also has antifungal props

toxicity: GI distress, teratogenic

drug interaction:

• H2 and PPIs that decrease gastric acid secretion
• drugs metabolized by P450s

Question 14

triconazoles

fluconazole

Answer 14

oral admin

• well absorbed, not affected by gastric acidity

wide distribution (incl CSF)

long halflife (25-30h)

fewest effects on hepatic microsomal enzymes (less drug ints)

wide therapeutic index

Question 15

triconazoles

voriconazole

posaconazole

Answer 15

newest triazoles

improved bioavailability

posaconazole : broadest spectrum

Question 16

drugs for systemic infections

echinocandins

• basics
• clinical use
• resistance

Answer 16

newest antifungals

semi-synth, water-sol, lipopeptide derivative of pneumocandin B

taken parenterally

ex. caspofungin (first to market), micafungin, anidulafungin

clinical uses

• Candida inf
• invasive Aspergillosis that survives amphoB

adverse effects

• fever, nausea, flushing, vomiting

resistance

• mutation in FKS1 = resistance

caspofungin mech of action: disruptor of cell wall

• inhibits beta1,3glucan synthase (FKS1)

Question 17

fungal cell wall

Answer 17

3 layers:

• mannoproteins
• layers of beta1,3glucan + beta1,6glucan
• chitin

*beta1,3glucan synthase is an enzyme in the cell membrane

• caspofungin inhibits beta1,3glucan synthase → depletes beta1,3glucans in cell wall → disrupts integrity of cell wall → lysis!

Question 18

drugs for systemic mucocutaneous infections

terbinafine

• basics
• clinical use
• advantage
• adverse effects
• drug ints

Answer 18

synthetic allylamine

synergistic with triazoles

mechanism : blocks ergosterol biosynth

• inhibits squalene epoxidase → blocks ergosterol synth → toxic accumulation of sterol squalene

advantage : accumulates in skin, nails, fat → prevents nail/skin superficial infection!

must be used continuously until inf clears

minimal side effects (GI distress, headache)

no significant drug ints

Question 19

drugs for topical infections

• creams, ointments, suppositories, lozenges

nystatin

Answer 19

topical amphotericin derivative

mechanism: ergosterol binder, pore former

admin: creams, ointments

clinical use: local suppression of candidal inf

Question 20

drugs for topical infections

• creams, ointments, suppositories, lozenges

terbinafine

Answer 20

mechanism: squalene epoxidase inhibitor

clinical use: dermatophyte-caused tinea

Question 21

drugs for topical infections

• creams, ointments, suppositories, lozenges

clotrimazole

miconazole

Answer 21

clinical use:

• oral, vulval candidiasis
• dermatophyte inf