Tyrvaya
Tyrvaya
Generic Name
Tyrvaya
Mechanism
- Receptor blockade: Competitive inhibition of ATP‑binding sites on VEGFRs, FGFRs, PDGFR‑α, KIT, and RET.
- Anti‑angiogenic effect: Reduces vascular endothelial growth factor–mediated neovascularization, starving tumors of oxygen and nutrients.
- Growth‑signal suppression: Blocks fibroblast growth factor signaling and downstream pathways (RAS/MAPK, PI3K/AKT), curbing tumor cell proliferation and survival.
- Tumor micro‑environment modulation: Inhibits stromal support through PDGFR‑α blockade, disrupting the tumor micro‑environment and enhancing TKI efficacy.
Pharmacokinetics
| Parameter | Value | Notes |
| Absorption | Oral; peak plasma 4–9 h post‑dose. | Food increases exposure by ~30 %. |
| Bioavailability | ~65 % | Oral formulation. |
| Distribution | Volume of distribution ~200 L | Highly protein‑bound (~97 %). |
| Metabolism | Primarily CYP3A4/5-mediated | Co‑administration with CYP3A4 inhibitors/inducers alters exposure. |
| Half‑life | ~19–23 h | Steady state achieved in ~2–3 weeks. |
| Excretion | Fecal (~78 %) and renal (~19 %) | Minimal renal clearance; caution in severe hepatic impairment. |
Indications
- Metastatic Renal Cell Carcinoma (mRCC) after progression on other TKI or immune therapy.
- Radioactive‑iodine refractory differentiated thyroid cancer (RET/FKFR‑mutant tumors).
- Unresectable neuroendocrine tumors (clinical trials ongoing).
Dosing
- Standard adult dose: 20 mg orally once daily in 28‑day cycles; hold 3 days for safety on days 1–3 if any grade‑3/4 toxicity develops.
- Hepatic impairment:
- Child‑Pugh B: 15 mg daily.
- Child‑Pugh C: Not recommended.
- Renal impairment: No dose adjustment required; reduce if CrCl < 30 mL/min and liver function compromised.
- Drug interactions: Avoid strong CYP3A4 inhibitors (ketoconazole, itraconazole) or inducers (rifampin, carbamazepine).
- Timing: Take with food; avoid alcohol.
Adverse Effects
- Common (≥ 10 %):
- Hypertension (31 %)
- Fatigue (29 %)
- Diarrhea (27 %)
- Nausea (17 %)
- Decreased appetite (12 %)
- Weight loss (10 %)
- Rash (8 %)
- Serious (≥ 1 %):
- Grade ≥ 3 hypertension (3 %)
- Proteinuria (2 %)
- Severe liver injury (1 %)
- GI perforation/fistula (≤ 0.5 %)
- Cardiac events (≥ 0.1 %)
Monitoring labs: CBC, CMP, liver enzymes, KFTs before each cycle; adjust dose for any Grade ≥ 3 toxicity.
Monitoring
- Blood pressure: Baseline, weekly for first month, then monthly.
- Liver function tests (ALT, AST, bilirubin): Baseline, at weeks 4, 8, 12, then every 2–3 months.
- Renal function (eGFR): Every cycle.
- Ultrasound/MRI scans: Every 8–12 weeks to evaluate tumor response per RECIST.
- Proteinuria screen: Urinalysis at baseline and every 4 weeks.
Clinical Pearls
- Start‑up dosing: 20 mg daily; consider 15 mg in patients on concomitant CYP3A4 inhibitors to avoid toxicity.
- Hypertension strategy: Initiate antihypertensives proactively; use ACEI/ARB or calcium‑channel blocker as first line.
- Re‑dose timing: Resume at full dose only after grade 2 or lower adverse events resolve; use a “step‑down” schedule (15 mg → 10 mg → 5 mg) if intolerable.
- Drug‑drug interactions: Lenvatinib markedly increases plasma levels of drugs metabolized by CYP3A4, so monitor therapeutic drug levels (e.g., tacrolimus).
- Patient education: Emphasize adherence, regular BP monitoring, prompt reporting of any GI bleeding or sudden flank pain (signs of GI perforation or renal injury).
- Efficacy beyond mRCC: Consider lenvatinib in combination with pembrolizumab for certain urothelial cancers; ongoing trials are expanding its therapeutic spectrum.
Quick Reference
• Brand: Tyrvaya (lenvatinib)
• Class: Multitargeted TKI (VEGFR/FGFR/PDGFR/Kit/RET)
• Key Action: Inhibits angiogenesis & tumor growth signaling
• Dose: 20 mg PO qd
• Major toxicity: Hypertension, fatigue, diarrhea, proteinuria
• Monitoring: BP, LFTs, renal function, imaging
*Use this drug card as a concise reference for both academic study and bedside clinical decision making.*