You are taking care of a patient with renal failure secondary to anti-fungal therapy. The patient is a 66-year-old male being treated for cryptococcal meningitis. This drug has a variety of known side effects including acute febrile reactions to infusions, anemia, hypokalemia and hypomagnesemia. What is the mechanism of action of this drug?

Pore formation secondary to ergosterol binding

Inhibition of squalene epoxidase

Disruption of microtubule formation

Inhibition of 1,3-beta-glucan synthase

An 18-year old college freshman presents to his university clinic because he has not been feeling well for the past two weeks. He has had a persistent headache, occasional cough, and chills without rigors. The patient’s vital signs are normal and physical exam is unremarkable. His radiograph shows patchy interstitial lung infiltrates and he is diagnosed with atypical pneumonia. The patient is prescribed azithromycin and takes his medication as instructed. Despite adherence to his drug regimen, he returns to the clinic one week later because his symptoms have not improved. The organism responsible for this infection is likely resistant to azithromycin through which mechanism?

Methylation of ribosomal binding site

Decreased binding to RNA polymerase

You are treating a neonate with meningitis using ampicillin and a second antibiotic, X, that is known to cause ototoxicity. What is the mechanism of antibiotic X?

It binds the 30S ribosomal subunit and inhibits formation of the initiation complex

It binds the 50S ribosomal subunit and inhibits formation of the initiation complex

It binds the 30S ribosomal subunit and reversibly inhibits translocation

It binds the 50S ribosomal subunit and inhibits peptidyltransferase

It binds the 50S ribosomal subunit and reversibly inhibits translocation

A pharmaceutical company is studying a new drug that inhibits the glucose transporter used by intestinal enterocytes to absorb glucose into the body. The drug was designed such that it would act upon the glucose transporter similarly to how cyanide acts upon cytochrome proteins. During pre-clinical studies, the behavior of this drug on the activity of the glucose transporter is examined. Specifically, enterocyte cells are treated with the drug and then glucose is added to the solution at a concentration that saturates the activity of the transporter. The transport velocity and affinity of the transporters under these conditions are then measured. Compared to the untreated state, which of the following changes would most likely be seen in these transporters after treatment?

Unchanged Km and decreased Vmax

Unchanged Km and unchanged Vmax

Increased Km and unchanged Vmax

Increased Km and decreased Vmax

Decreased Km and decreased Vmax

A 31-year-old female receives a kidney transplant for autosomal dominant polycystic kidney disease (ADPKD). Three weeks later, the patient experiences acute, T-cell mediated rejection of the allograft and is given sirolimus. Which of the following are side effects of this medication?

Hyperlipidemia, thrombocytopenia

Nephrotoxicity, gingival hyperplasia

Cytokine release syndrome, hypersensitivity reaction

Flucytosine for USMLE Step 1: High-Yield Pharmacology Lessons

Mechanism of Action - Fungal DNA Faker

Selective Uptake: Enters fungal cells via cytosine-specific permease.
Lethal Conversion: Inside the fungus, it's converted to its active forms.

DNA Block: 5-FdUMP inhibits thymidylate synthase, blocking dTMP synthesis and halting DNA production.
RNA Disruption: 5-FUTP is incorporated into fungal RNA, disrupting protein synthesis.

⭐ Selective Toxicity: Human cells lack cytosine deaminase, preventing the conversion of Flucytosine to toxic 5-FU, which is a key reason for its antifungal selectivity.

Antifungal mechanisms of action on fungal cell

📌 Mnemonic: Flucytosine → Fake Uracil → Faulty DNA/RNA.

Clinical Spectrum & Use - The Amphotericin Ally

Narrow-spectrum fungistatic; resistance develops rapidly when used as monotherapy.
Primary Targets:
- Cryptococcus neoformans
- Some Candida spp.
- Molds causing chromoblastomycosis.
Key Strategy: Used synergistically with Amphotericin B.
- Amphotericin B creates pores in the fungal membrane, which ↑ flucytosine entry.
- This combination allows for lower, less toxic doses of Amphotericin B.
Main Indication:
- Severe systemic infections, particularly cryptococcal meningitis.

⭐ The synergy is key: Amphotericin B opens the "door" (cell membrane pores), letting Flucytosine enter the fungal cell to inhibit DNA/RNA synthesis.

Pharmacokinetics - Body's Drug Tour

Absorption: Well-absorbed orally (>90% bioavailability).
Distribution:
- Distributes widely into body tissues and fluids.
- Excellent penetration into the CSF (~75% of serum levels).
- Low plasma protein binding.
Metabolism: Minimal host metabolism. Gut flora can convert it to 5-fluorouracil (5-FU), contributing to toxicity.
Excretion:
- Primarily renal; >90% excreted unchanged in urine.
- ⚠️ Dose reduction is critical in renal insufficiency.

⭐ Its ability to penetrate the CNS makes it vital for treating fungal meningitis, especially cryptococcal, typically in combination with Amphotericin B.

Adverse Effects - Bone Marrow Blues

Primary Toxicity: Dose-dependent bone marrow suppression.
Mechanism: Intestinal flora convert flucytosine to the antimetabolite 5-fluorouracil (5-FU), a potent myelosuppressant.
- Inhibits thymidylate synthase, disrupting DNA and RNA synthesis in hematopoietic stem cells.
Manifestations:
- Anemia (↓ RBCs)
- Leukopenia (↓ WBCs) → risk of infection
- Thrombocytopenia (↓ Platelets) → risk of bleeding

⭐ High-Yield: Toxicity is markedly increased in patients with renal insufficiency due to drug accumulation. Always monitor plasma levels and renal function.

Flucytosine mechanism of action and toxicity

Resistance - Fungal Escape Plan

Altered uptake: Mutation in fungal cytosine permease reduces drug entry.
Impaired metabolism: Deficient cytosine deaminase or UMP pyrophosphorylase prevents conversion to active metabolites (5-FU, FdUMP).

⭐ Resistance develops rapidly with monotherapy. Always combine, usually with Amphotericin B for synergistic effect.

High‑Yield Points - ⚡ Biggest Takeaways

Converted to 5-fluorouracil (5-FU) in fungal cells, which inhibits DNA and RNA synthesis by blocking thymidylate synthase.

Almost always used in combination with Amphotericin B, especially for severe systemic mycoses like cryptococcal meningitis.

Amphotericin B enhances flucytosine uptake into fungal cells, creating a synergistic effect.

Rapid resistance develops when used as monotherapy.

Main adverse effect is bone marrow suppression due to systemic conversion to 5-FU.

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Flucytosine