Tretinoin

Topical, oral (APL only)

Topical: irritation within days; acne improvement 6-12 weeks; oral APL response within days

N/A

~0.5-2 hours (oral)^[1]

Topical: minimal systemic absorption with normal skin; oral: variable, induced metabolism with repeated dosing^[1]

Oral tretinoin is teratogenic (Category D historically; APL exception treated under strict pregnancy avoidance); topical tretinoin in pregnancy has lower (but not zero) concern and is generally avoided.^{[citation needed]}

Rx-only in US

Tretinoin is all-trans retinoic acid, the active metabolite of vitamin A; it binds nuclear retinoic acid receptors (RAR α/β/γ), regulating transcription of genes governing epithelial differentiation, proliferation, and inflammation.▲0▼ In acne, normalizes follicular keratinization and reduces comedone formation. In APL, the PML-RARα fusion oncoprotein responds to pharmacologic ATRA by resuming terminal granulocytic differentiation — one of the first successful examples of differentiation therapy in oncology, transforming APL from highly fatal to highly curable. Differentiation syndrome (capillary leak, hyperleukocytosis, dyspnea) is the major adverse effect of oral APL induction^[1].