- Class: Alkylating agent (nitrogen mustard derivative).
- Historical note: First anticancer chemotherapy drug (developed from WWI chemical warfare agents).
Mechanism of Action (MOA)
- Highly reactive bifunctional alkylating agent.
- Forms aziridinium ion intermediates that alkylate DNA at the N7 position of guanine.
- Results in intra- and inter-strand crosslinks → inhibition of DNA replication and transcription → apoptosis.
- Non–cell cycle specific.
Clinical Uses
- Historically in Hodgkin and non-Hodgkin lymphomas (part of the classic MOPP regimen: Mechlorethamine, Oncovin [vincristine], Procarbazine, Prednisone).
- Rarely used today due to toxicity and better alternatives.
- Topical mechlorethamine (Valchlor® gel, 0.016%) → used for cutaneous T-cell lymphoma (CTCL, e.g., mycosis fungoides).
Dosing
- IV (historical use in lymphoma): 0.4 mg/kg IV every 4 weeks (in MOPP regimen).
- Topical: 0.016% gel once daily to affected skin areas (Valchlor®).
Toxicities
- Severe myelosuppression (dose-limiting).
- Nausea/vomiting (very emetogenic).
- Alopecia, mucositis.
- Extravasation → severe local necrosis (highly vesicant).
- Secondary malignancies (especially leukemias).
- Topical: contact dermatitis, pruritus, erythema, skin ulceration.
Monitoring
- CBC (bone marrow suppression).
- Skin exam if topical (dermatitis, ulceration).
- Extravasation precautions with IV.
Summary
Mechlorethamine is the prototype nitrogen mustard alkylating agent. Rarely used IV now due to high toxicity, but still relevant topically in cutaneous T-cell lymphoma (Valchlor®). Main concerns: myelosuppression, vesicant injury, and secondary malignancies.