Generic Name

Venclexta

Mechanism

• Potent, selective inhibitor of BCL‑2 – binds the BH3 domain of BCL‑2, displacing pro‑apoptotic proteins (BAX, BAK) and triggering mitochondrial outer‑membrane permeabilization.
• Overcomes anti‑apoptotic signaling in malignant B‑cell clones and AML blasts, restoring apoptotic priming that is otherwise suppressed in disease.
• Synergistic when combined with hypomethylating agents (decitabine) or with anti‑CD20 antibodies (rituximab).

Pharmacokinetics

Indications

• Chronic lymphocytic leukemia (CLL) / Small lymphocytic lymphoma (SLL) in patients with ≥ 1 prior therapy (≥ 1‑cycle of ibrutinib/venetoclax‑based regimens).
• CLL/SLL with del(17p)/TP53 mutation after at least one prior therapy.
• Relapsed/refractory acute myeloid leukemia (AML) in patients ≥ 75 yr or unfit for intensive chemotherapy.
• Combination indications: with obinutuzumab (CLL) or rituximab (C‑LL) and with hypomethylating agents (AML).

Contraindications

• Absolute contraindication: Known hypersensitivity to venetoclax.
• Risk for Tumor Lysis Syndrome (TLS): High tumor burden (e.g., >20 % marrow blasts, >10 % peripheral leukocyte count).
• Caution with: Severe neutropenia, high lactate dehydrogenase (LDH), active infections, concurrent use of strong CYP3A4/2J inducers.
• Special warnings:
• Severe myelosuppression → need for growth factor support.
• Cardiac toxicities: Monitor QTc; avoid in patients with existing prolonged QTc or on QT‑prolonging drugs.

Dosing

1. Dose Ramp‑up (CLL)

2. Dose Ramp‑up (AML) – similar 7‑day ramp, then 400 mg daily.

3. Combination therapy:
• With rituximab: start venetoclax on Day 3 of rituximab, maintain 400 mg daily.
• With hypomethylating agents: 400 mg daily, 5 days per 28‑day cycle (decitabine/azacitidine).

4. Administration: take orally with minimal food; avoid high‑fat meal on the first dose.

5. Re‑dosing after interruption: if missed ≥ 24 h, repeat ramp‑up.

Adverse Effects

Monitoring

• Baseline: CBC with diff, CMP, LDH, electrolytes, QTc, infection screen, renal/hepatic function.
• During ramp‑up: Daily CBC on days 1–8; monitor for TLS (serum electrolytes, uric acid).
• After therapy initiation:
• CBC: weekly (weeks 0‑7), then biweekly (months 2‑4), then monthly.
• LDH and CRP: every cycle.
• QTc: at baseline and twice weekly during ramp.
• Tumor burden assessment (CT/US) every 2‑3 cycles.
• Infections: Regular screening; consider prophylaxis (valganciclovir, acyclovir).
• Growth factor support: G‑CSF if ANC < 0.5 × 10⁹/L.

Clinical Pearls

• “Rule of 7”: Start with 7 days of ramp‑up to minimize TLS; adjust if creatinine or liver function changes.
• Avoid strong CYP3A4 inducers (e.g., rifampin, St. John’s wort) at any time—dose reductions of up to 75 % required.
• Use a *watch‑and‑wait* TLS protocol: high‑risk patients (>25 % lymphocytes, LDH >2× ULN) get prophylactic allopurinol, aggressive hydration, and can begin venetoclax at 20 mg with escalation later.
• Combine with rituximab or obinutuzumab to prevent early resistance: start rituximab on Day 1, ramp venetoclax later; this synergy boosts overall response rates in CLL.
• When in refractory AML, keep treatment short (≤ 4 cycles) unless using ongoing combination with hypomethylating agents; many patients respond only after 2–3 cycles.
• Key diagnostic tip: A marked drop in LDH and peripheral blast count in the first 4 weeks is a surrogate for early response; lack of decline may prompt dose adjustment or combination change.
• Patient education point: Stress the importance of reporting new fever, dizziness, or ECG changes promptly—early TLS detection saves lives.

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• References

1. National Comprehensive Cancer Network (NCCN) Guidelines for CLL/AML, v2.2025.

2. Armand P, et al. *Lancet Oncol.* 2019;20(5): 663–672.

3. BCL‑2 Inhibitors: Clinical Pharmacology & Practice, 2024.

*Prepared for medical students and practicing clinicians seeking a quick, evidence‑based reference to Venclexta (venetoclax).*