Lecture 19 Antifungal Drugs PDF

Summary

This lecture covers antifungal drugs, including learning objectives, classification of fungal infections, and the mechanism of action for different antifungal drug classes. Key topics discussed include the prevalence of fungal infections, core concepts, challenges, and potential toxicities associated with their use.

Full Transcript

PHAR2210 Foundations of Pharmacology

Lecture 19 Antifungal drugs

Dr Ricky Chen

Chapter 54, Rang & Dale's Pharmacology (Tenth Edition, 2023)
 Learning outcomes
After completing this lecture, you should be able to
list factors that contribute to the increased prevalence of fungal infections
describe the classification of mycoses and the relevant site of infection
describe the pharmacokinetics, mechanism of action, and adverse effects of each of the
four antifungal drug classes and provide an example for each drug class
Core concepts of pharmacology
pharmacodynamics pharmacokinetics
Drug-target Drug target
Steady-state Drug absorption Drug bioavailability
interaction
concentration
Mechanism of Structure-activity Drug distribution Volume of distribution
drug action relationship Zero- and first-
order kinetics Drug metabolism Drug clearance
Affinity Drug selectivity
Drug elimination Drug elimination half-life
Potency Efficacy
DRUG

Dose/concentration- Drug tolerance
response relationship
Therapeutic index
Adverse drug reaction
Individual variation
Adapted from Guilding et al. (2023) Defining and
Drug interaction in drug response unpacking the core concepts of pharmacology: A global
initiative. British Journal of Pharmacology, 1-18.
Patient outcomes https://doi.org/10.1111/bph.16222
 Fungi
fungi are eukaryotic cells​; ~100,000 species classified, estimates between 1.5 and 5.1 millions​
present in the environment or may coexist with humans as commensals​
a limited number of species are pathogenic in humans

Yeasts
grow as unicellular form
Moulds
grow as multicellular filaments (hyphae) → branch to
form a network (mycelium)​
Dimorphic fungi
assume either filamentous or yeast-like morphology
depending on the environment​

Sudbery (2011)
 Two sides of fungi
consumption (e.g., mushrooms)
Good
manufacturing (e.g., Baker’s yeast in beer making; antibiotic production)
damages to animals, crops or food
fungal diseases in humans - cost > $7.2 billion in 2017 in the USA (Benedict et al., 2019)
Bad
o Candida infections and Aspergillus infections
o dermatophyte infections responsible for over half of outpatient visits

Most fungal infections are opportunistic infections
rarely cause disease in healthy individuals
nonpathogenic fungi become pathogenic in immunocompromised patients
Increasing prevalence of fungal infections
widespread use of broad-spectrum antibiotics - eliminate nonpathogenic bacterial competitors
use of immunosuppressant
AIDS
cancer chemotherapy
diabetes
Fungal infections (mycoses)

Classification Site of infection​
outermost epidermal layer of
superficial skin (i.e., stratum corneum) or
outer surface of hair shafts​
epidermal layer of skin, hair
cutaneous
shafts, and nails​
dermal and underlying layers of
subcutaneous
skin​ modified from Kabashima et al. (2019)

serious infections of internal organs​ - gain access via the respiratory tract, the GI
systemic tract, or blood vessels​
primary vs. opportunistic pathogens
 Antifungal (antimycotic) drugs
Challenges
biological similarities between humans and fungi as eukaryotes
can be toxic to host (oral antifungal drugs must be strictly monitored)
distinctive sterols: ergosterol in fungal cell membranes vs. cholesterol in human cells

Timeline of systemic antifungal drugs (Lewis, 2011)
 Antifungal (antimycotic) drug classes
route of administration (oral/topical/intravenous) - drug absorption from the GI tract?
dosing strategies - ↑ drug efficacy and ↓ risk of toxicity
spectrum of action (yeasts/moulds/dimorphic)
site of infection
renal/hepatic clearance
drug-drug interaction

inhibit cell wall synthesis
o echinocandins* (semisynthetic)
alter cell membrane integrity or permeability
o polyenes* (natural occurring)
o allylamines* (synthetic)
o azoles* (synthetic)
Volmer et al. (2010)
Fungal cell wall
cell wall structure of selected fungal cells

Erwig and Gow (2016)
 Echinocandins
-fungin (e.g., caspofungin)
o synthetic modification of echinocandin B (a hexapeptide + lipid side chain)
bind to β-1,3-glucan synthase → inhibit β-1,3-glucan synthesis​

echinocandin B

poor oral absorption - i.v. administration
concentration-dependent activity - Cmax:MIC
fungicidal for Candida species - treat invasive candidiasis
fungistatic for Aspergillus species
nausea, vomiting and diarrhoea
infusion-related reactions
Brown et al. (2011)
 Polyenes
natural products - broad-spectrum antifungal macrolides
interaction with ergosterol is key to antifungal activity
o ergosterol in fungi - regulation of cellular process; membrane stability and fluidity
o form pores - leakage of intracellular contents, e.g., K+ ions
o interactions at the surface of cell membranes

Carolus et al. (2020)
Polyenes
Amphotericin B*
broad spectrum - most fungi and yeasts

poor oral absorption
o treat infection of the upper GI tract amphotericin B
o systemic infection - slow i.v. infusion
minimal hepatic metabolism
o mainly faecal elimination

infusion-related - inflammatory response
nephrotoxicity - interactions with cell membranes
liposomal formulations - ↓ toxicity

Gray et al. (2012)
Inhibition of ergosterol biosynthesis
squalene

squalene monooxygenase allylamines*

2,3-oxidosqualene

lanosterol
cell membrane stability and fluidity
14-demethylase azoles*

4,4-dimethyl-Δ8,14,24-trienol 4,4-dimethyl-Δ8,24-dienol
X
ergosterol
 Allylamines
synthetic fungicidal antifungal drugs
squalene
squalene monooxygenase allylamines*
2,3-oxidosqualene terbinafine

terbinafine*
treatment for onychomycosis (fungal infection of the nail bed, matrix, or plate)
o major cause of infection - dermatophytes (e.g., Trichophyton rubrum)
o highly lipophilic and keratinophilic - dermatophytes require keratin for growth
oral or topical administration - rapid absorption and is taken up by skin and nails
CYP2D6 inhibitor - potential drug-drug interaction

GI disturbance
rash
muscle pain
 Azoles
broad-spectrum synthetic fungistatic drugs
lanosterol
14-demethylase azoles*

4,4-dimethyl-Δ8,14,24-trienol

imidazoles
Lewis (2011)
e.g., ketoconazole - first azole administered orally to treat systemic infections
triazoles
e.g., itraconazole* itraconazole
 Azoles
itraconazole*
can be administered orally but absorption is variable
extensive hepatic metabolism
GI disturbance
hepatotoxicity
cardiotoxicity - QT interval prolongation
a CYP3A4 inhibitor - drug-drug interaction

midazolam CYP3A4 1-hydroxymidazolam

midazolam following itraconazole pretreatment (▲)
midazolam 4 days after itraconazole pretreatment (∆)
midazolam alone (○)

Backman et al. (1998)
Antifungal drug-related toxicities

Lewis (2011)