Generic Name

Lenvima

Mechanism

• Multitarget inhibition: blocks VEGFR‑1/2/3, FGFR1‑4, PDGFR‑α, KIT, and RET signaling pathways.
• Anti‑angiogenic: inhibits endothelial cell proliferation and new vessel formation, reducing tumor blood supply.
• Direct tumor cell effects: inhibits growth factor receptors on tumor cells, inducing apoptosis and growth arrest.
• Impressive downstream blockade: suppression of the MAPK/ERK and PI3K/AKT pathways, essential for tumor survival.

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Pharmacokinetics

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Indications

• Unresectable, locally advanced, or metastatic radio‑iodine‑refractory differentiated thyroid cancer *(first‑line systemic therapy)*.
• Unresectable, symptomatic, or metastatic hepatocellular carcinoma (first‑line systemic therapy).
• Investigational use: renal cell carcinoma (phase III), anaplastic thyroid cancer (phase I/II).

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Contraindications

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Dosing

• Standard dose: 12 mg orally once daily (with or without food).
• Initial treatment: 12 mg for thyroid cancer; 12 mg for HCC.
• Dose adjustment: Down‑titrate by 4 mg increments (to 8 mg or 4 mg) for intolerance or adverse events; up‑titrate only in select scenarios.
• Storage: 15 – 30 °C (room temperature), protected from light.
• Missed dose: If < 8 h since the last dose, take the missed dose; otherwise skip and resume next scheduled dose.

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Adverse Effects

Common (≥10 %)
• Hypertension
• Fatigue
• Diarrhea
• Decreased appetite / weight loss
• Nausea / vomiting
• Anorexia
• Proteinuria
• Headache
• Arthralgia / myalgia

Serious (≥1 %)
• Hypertensive Crisis
• Severe proteinuria → possible nephrotic syndrome
• Bleeding (gastrointestinal, epistaxis, hemoptysis)
• Cardiac events (heart failure, arrhythmias)
• Impaired wound healing (post‑operative)
• Severe liver dysfunction (transaminitis)

Monitoring

• Blood pressure: ≥ twice weekly, especially after dose changes.
• Urine output and proteinuria: urinalysis at baseline, monthly, and when clinically indicated.
• Liver function tests: baseline, week 4, then every 4 weeks.
• Platelet count & coagulation profile: baseline, every 4‑6 weeks.
• Electrocardiogram (ECG): baseline, as clinically indicated (QTc).
• Pregnancy test: baseline and every 3 months.

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Clinical Pearls

• “Off‑by‑Clock” dose‑timing matters: A 12‑hr delay can be clinically significant; counsel patients on strict daily timing.
• CYP3A4 interplay: Ketoconazole, ritonavir dramatically ↑ lenvatinib levels; rifampin may restore too low. Adjust dose or monitor closely.
• Hydration & proteinuria: Encourage adequate fluid intake (≥2 L/day) to dilute urinary protein excretion.
• Hypertension management: Add or titrate an ACE inhibitor or ARB; avoid non‑steroidal anti‑inflammatory drugs that may worsen proteinuria.
• Bleeding risk with surgery: Discontinue lenvatinib ≥4 weeks pre‑op; resume 2‑4 weeks post‑op or per surgical protocol.
• Comparative advantage vs. sorafenib: Lenvatinib offers higher objective response rates in HCC but a higher incidence of proteinuria; suitable patient selection is key.
• Use in thyroid cancer: The benefit is largely progression‑free survival (PFS); monitor Tg levels to gauge response early.
• Patient education: Emphasize reporting early signs of bleeding, proteinuria (dark urine), and uncontrolled BP.

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• References
• GLOBOCAN 2023, ESMO Clinical Practice Guidelines, FDA label (Lenvima, 2023).
• J. Clin. Oncol. 2020;38:723‑734 (lenvatinib for HCC).
• Thyroid 2021;31:1143‑1155 (lenvatinib in RAI‑DTC).

*Use this drug card as a quick reference; consult the product label and the latest clinical trials for comprehensive guidance.*