Generic Name

Mylotarg

Mechanism

• Target: CD33 receptor expressed on >90 % of AML blasts.
• Binding & Internalization: The antibody binds CD33 → receptor‑mediated endocytosis.
• Linker Cleavage: Inside the lysosome, a hydrazine‑based linker is cleaved.
• Drug Release: The small‑molecule cytotoxic auristatin G is released, inhibiting microtubule polymerization.
• Cell Death: Disruption of microtubules → mitotic arrest → apoptosis of the leukemic cell.

This targeted delivery preserves normal marrow cells while maximizing cytotoxicity to AML blasts.

Pharmacokinetics

> Clinical Tip: No dose adjustment required for mild–moderate renal impairment; avoid in severe renal failure (CrCl < 30 mL/min) pending further data.

Indications

• Acute myeloid leukemia (AML) –
• Newly diagnosed, unfit for intensive chemotherapy or as salvage therapy.
• First‑line in combination with cytarabine ± anthracycline (e.g., 7 + 3).
• Post‑remission consolidation in high‑risk cytogenetic AML (except t(15;17)).

> Off‑label: Consider in relapsed/refractory AML where no standard options remain.

Contraindications

• Contraindicated in patients with:
• Known hypersensitivity to gemtuzumab‑ozogamicin or murine proteins.
• Active infections precluding immunosuppression.
• Warnings:
• Veno‑occlusive disease (VOD)—especially post‑bone‑marrow transplant.
• Immune‑mediated cytokine release syndrome (CRS)—may mimic sepsis.
• Hepatotoxicity & transaminitis.
• Toxic epidermal necrolysis / Stevens–Johnson syndrome in severe reactions.
• Precautions:
• Avoid in pregnancy and lactation (category X).
• Use with caution in patients with pre‑existing liver disease or ongoing drug interactions that may affect albumin levels.

Dosing

• Pre‑medication: Antipyretic (acetaminophen) ± antihistamine 30 min before infusion.
• Monitoring: Baseline CBC, CMP, bilirubin; repeat CBC ≥ daily for 14 days, CMP weekly.
• Infusion Duration: 90 min for first dose; 60 min for subsequent.

> Important: Do not exceed 6 cumulative cycles; dose escalation beyond 6 is not FDA‑approved.

Adverse Effects

• Common (≥10 %)
• Neutropenia, thrombocytopenia
• Fever, chills, infusion‑related reactions
• Nausea, vomiting, constipation
• Fatigue, anorexia
• Serious (≤10 %)
• Veno‑occlusive disease of the liver (VOD) – 5–10 %
• Cytokine release syndrome (CRS) – 3–5 %
• Severe hepatotoxicity (ALT/AST ↑ >5× ULN) – 2–3 %
• Drug reaction with eosinophilia and systemic symptoms (DRESS) – < 1 %
• Cardiac arrhythmias (rare)
• Late‑onset
• Secondary malignancies (e.g., acute lymphoblastic leukemia) Management:

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• Administer tocilizumab or steroids for CRS.

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• Treat VOD with defibrotide if early signs appear.

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• Supportive care for cytopenias.

Monitoring

> Alert: Patients with baseline bilirubin > 2 mg/dL are at increased VOD risk; consider dose reduction or defer therapy.

Clinical Pearls

• Infusion Speed Matters: Faster infusions (>45 min) increase CRS risk; slow the rate to ≤2 h.
• Bilirubin Check: A pre‑infusion bilirubin > 2 mg/dL is a red flag; consider switching to alternative AML regimens.
• Post‑Transplant VOD: Avoid Mylotarg within 30 days pre‑ or post‑stem cell transplant unless absolutely required.
• Combination with Idarubicin: Studies suggest synergistic benefit, but vigilance for overlapping cardiotoxicity.
• Adjuvant Therapy: Pairing Mylotarg with low‑dose cytarabine extends overall survival in older adults (≥60 y).
• Patient Education: Emphasize signs of VOD (painful hepatomegaly, weight gain, jaundice) and CRS (fever, hypotension).
• Drug–Drug Interactions: Minimal CYP involvement; watch for drugs affecting albumin levels that may alter free drug fraction.

> These pearls help tailor Mylotarg therapy safely to the most vulnerable AML patients while minimizing life‑threatening complications.