Gavreto
Gavreto
Generic Name
Gavreto
Mechanism
- Selective inhibition of mutant BRAF V600 tyrosine‑kinase, blocking downstream MEK‑ERK signaling.
- Restores normal proliferation control in melanoma cells, leading to apoptosis and tumor regression.
- When combined with the MEK inhibitor binimetinib, continuous blockade of the MAPK pathway reduces compensatory signaling and limits resistance.
Pharmacokinetics
- Form: Oral tablets (300 mg).
- Absorption: Rapid, peak plasma concentration (Tmax) within 3–4 h after dosing.
- Bioavailability: ~55 % after a single 300‑mg dose; food increases exposure modestly.
- Distribution: Extensive; protein binding ~95 % (predominantly to albumin).
- Metabolism: Primarily CYP3A4/5 mediated, with minor involvement of CYP1A2 and UGT1A9.
- Elimination: ~70 % excreted in feces, 25 % in urine; mean half‑life 10–12 h.
- Drug interactions: Strong CYP3A4 inhibitors/inducers alter exposure; co‑administration with digoxin or other CYP3A substrates warrants monitoring.
Indications
- Metastatic or unresectable melanoma with confirmed BRAF V600E/K mutation in combination with binimetinib (BRAF + MEK inhibitor therapy).
- Approved for patients aged ≥18 y; no validated indication in pediatric/adolescent populations.
Contraindications
- Contraindicated with strong CYP3A4 inhibitors (e.g., clarithromycin, ketoconazole) when taken with binimetinib.
- Warnings:
- Photosensitivity reactions; patients advised to use sunscreen; photoprotective clothing.
- Potential for cutaneous squamous cell carcinoma and keratoacanthoma—regular dermatologic exams.
- Interstitial lung disease/pneumonitis—prompt evaluation for respiratory symptoms.
- Cardiac toxicity: QTc prolongation occasionally noted; baseline and periodic ECGs recommended.
- Abdominal pain may precede pancreatitis or acute cholangitis.
Dosing
- Standard dose: 300 mg PO once daily (300 mg tablet).
- When combined with binimetinib: binimetinib 45 mg PO twice daily, or 30 mg PO twice daily if high CYP3A activity or concomitant strong inhibitors.
- Start–stop guidelines: Initiate as soon as possible; if no therapeutic response or disease progression after 2–3 months, consider discontinuation.
- Overdose: No specific antidote; supportive care and monitoring.
Adverse Effects
| Adverse Effect | Incidence (≥+%) | Notes |
| Rash (maculopapular, pruritus) | 30–45 % | Treat with topical steroids/antihistamines; severe cases may need dose reduction. |
| Photosensitivity and photodermatitis | 25 % | Counsel on sun protection and use of broad‑spectrum sunscreen. |
| Fatigue | 20–30 % | Conservative measures and dose adjustment if limiting. |
| Nausea, vomiting, diarrhea | 15–25 % | Standard anti‑emetic prophylaxis and oral rehydration. |
| Elevated transaminases (≥3× ULN) | 8–12 % | Early discontinuation if >5× ULN or symptomatic cholestasis. |
| Pulmonary toxicity (pneumonitis) | 5–8 % | Suspect when dyspnea, cough, or fever develops. |
| Cardiovascular complications (QTc prolongation, reduced LVEF) | 4–6 % | Baseline ECG, monitoring after 2–3 weeks. |
| Keratoacanthoma & squamous cell carcinoma | <5 % | Baseline skin exam; biopsies at suspicious lesions. |
Monitoring
- Baseline: CBC, CMP (LFTs), ECG, dermatologic exam, pulmonary assessment.
- Ongoing:
- CBC/CMP every 2 weeks for first 2 months, then monthly.
- ECG at 4 weeks and if symptomatic.
- Skin surveillance monthly for lesions.
- Pulmonary evaluation (symptom check) at each visit.
- Therapeutic drug monitoring: Not routinely required unless drug interaction concerns.
Clinical Pearls
- Combination synergy: Encored with binimetinib exploits dual MAPK blockade, giving higher response rates (~60 %) vs BRAF‑only therapy (~30 %).
- Rapid onset: Patients can expect objective radiographic responses within 6–8 weeks; early imaging may help guide continuation strategy.
- Photosensitivity first: Often the earliest sign of toxicity—teach patients to check for rash after sun exposure.
- High‑risk patients: Those with pre‑existing cardiac dysfunction, liver disease, or on strong CYP3A inhibitors should receive intensified monitoring or alternative regimens.
- Adjuvant nature: In selected patients with resected metastatic melanoma, BRAF + MEK inhibitors are being explored as adjuvant therapy—clinical trial data emerging.
- Drug‑drug interactions: Avoid co‑administration of grapefruit juice, ketoconazole, or rifampin; provide patient counseling on over‑the‑counter meds.
Key Takeaway: Gavreto (encorafenib) paired with binimetinib delivers robust, MAPK‑pathway targeted therapy for BRAF‑mutant melanoma, but demands vigilance for photosensitivity, skin carcinogenesis, and cardiac/liver safety signals.