Afinitor | Pharmacology Mentor

Generic Name

Afinitor

Mechanism

mTOR Inhibition: Afinitor binds FKBP‑12 → inhibits mTOR complex‑1 (mTORC1) and mTORC2, disrupting downstream signaling involved in cell growth, proliferation, and angiogenesis.
Effects on the Cell Cycle: Induces G1‑phase arrest by down‑regulating Cyclin D1 and up‑regulating PTEN.
Impact on Tumor Microenvironment: Suppresses VEGF‑A production, reducing angiogenesis and tumor vascular supply.

Pharmacokinetics

Parameter	Typical Value	Notes
Absorption	95 % by mouth; peak 1–2 h (high‑fat meals ↑ peak 1.5‑2 h)	Oral bioavailability high; food increases absorption.
Distribution	Vol. Distrib. ≈ 1.2 L/kg (high plasma protein binding 89‑95 %)	Tissue penetration adequate (e.g., CNS).
Metabolism	Primarily CYP3A4‑mediated hepatic oxidation; also CYP2C19	Drug–drug interactions with strong CYP3A4 inhibitors/inducers.
Elimination	68 % biliary; 32 % renal	Half‑life ~30 h; steady‑state ≈ 14 days.
Special Populations	Adjust for hepatic impairment; no dose adjustment needed for mild–moderate renal impairment.	Severe hepatic impairment: avoid.

Indications

Advanced renal cell carcinoma (RCC) – first‑line therapy with or without interferon‑α.
Metastatic hormone‑positive HER2‑negative breast cancer – often combined with endocrine therapy.
Pancreatic neuroendocrine tumors (pNET) – as monotherapy or combination.
Subependymal giant cell astrocytoma in tuberous sclerosis complex (pediatric).
Approved pediatric use in specific CNS tumors with TSC.

Contraindications

Contraindications
• Known hypersensitivity to temsirolimus or any component.
• Severe hepatic impairment (Child‑Pugh C).

Warnings
• Pneumonitis – pulmonary infiltrates, dyspnea.
• Stomatitis / Oral ulcers – may preclude dosing.
• Impaired wound healing – avoid surgery up to 7 days prior/following therapy.
• Glycologic disturbance – hyperglycemia, hyperlipidemia → monitor and control.
• Infection risk – opportunistic infections; vigilance for sepsis.
• Torsades‑de‑pointes – due to QT prolongation in severe cases; monitor ECG in QT‑long patients.

Dosing

Adults (with adequate hepatic/renal function): 10 mg orally once daily.
Renal dysfunction (CrCl ≥ 50 mL/min): 10 mg daily.
Severe hepatic impairment: Avoid.
Pediatric (TSC): 2 mg/m² orally or IV, every 7 days (dose adjustable by weight).
Administration tips: Take with food to enhance absorption; avoid high‑fat meals if risk of hyperlipidemia; consistent 24‑h interval.
Ongoing assessment: Evaluate compliance and adherence; educate about potential GI upset.

Monitoring

Parameter	Frequency	Rationale
CBC, CMP	Every 2–3 weeks (first 2 months)	Detect neutropenia, liver injury
Blood glucose	Every 2–4 weeks	Prevent steroid‑like hyperglycemia
Lipid panel	Every 4 weeks	Mitigate pancreatitis risk
Chest X‑ray / HRCT (if respiratory symptoms)	On suspicion of pneumonitis	Early detection
ECG	Baseline; repeat if QT‑prolonging therapy added	Capture arrhythmias
Patient diary	Daily	Record mucositis, fatigue, appetite changes

Clinical Pearls

Start low, stay low: In patients on chronic steroids or with baseline lymphopenia, consider a 5‑mg daily starter dose, titrating to 10 mg when tolerated.
Food synergy: A high‑fat meal increases bioavailability; use this strategically in patients on lipid‑normalizing agents.
Pneumonitis sentinel: Even mild cough or shortness of breath warrants immediate imaging; early intervention with prednisone may avert dose‑limiting toxicity.
Infection prophylaxis: For high‑risk patients, consider prophylactic antivirals (eg, valacyclovir) and antifungals (fluconazole) during the first 3 months.
Breast‑cancer synergy: Combine with aromatase inhibitors to exploit complementary anti‑angiogenic and hormonal blockade pathways; monitor for overlapping endocrine side effects.
Pediatric dosing: Weight‑based dosing (2 mg/m² every 7 days) avoids over‑exposure; maintain a pediatric-specific monitoring bundle especially for TSC lesions.
Drug‑drug interactions: Concomitant potent CYP3A4 inhibitors (ketoconazole, clarithromycin) can raise temsirolimus exposure; use dose reduction or alternative antibiotics.

> Bottom line – Afinitor provides a valuable mTOR‑blocking strategy in advanced malignancies but requires vigilant monitoring for metabolic, pulmonary, and infectious complications. Early recognition of adverse events and proactive dose adjustments improve tolerance and therapeutic success.