AdapalenevsRetinol

Adapalene selectively binds RAR-beta and RAR-gamma (minimal RAR-alpha affinity), reducing inflammatory signaling compared to pan-RAR agonists. It normalizes follicular epithelial differentiation and reduces corneocyte cohesion in the pilosebaceous unit, preventing microcomedo formation. Adapalene inhibits AP-1 transcription factor (c-Fos/c-Jun dimerization), suppressing IL-6, TNF-alpha, and neutrophil chemotaxis. It promotes comedolysis by accelerating desquamation of existing comedones. For anti-aging, it stimulates fibroblast collagen I and III via RAR-beta/gamma, with comparable efficacy to tretinoin. Its lipophilic naphthoic acid structure confers superior follicular penetration and light stability.

Retinol undergoes two-step enzymatic conversion in keratinocytes: alcohol dehydrogenase (ADH) and retinol dehydrogenase (RDH) oxidize retinol to retinaldehyde; retinaldehyde dehydrogenase (RALDH) then oxidizes it to all-trans retinoic acid. Conversion is rate-limited by enzyme availability and CRBP expression, delivering retinoic acid gradually—explaining retinol's gentler profile. Only retinoic acid binds RAR/RXR receptors. Once converted, it activates identical pathways as tretinoin: upregulating keratinocyte proliferation, stimulating fibroblast collagen I/III via TGF-beta, inhibiting MMPs, and normalizing melanocyte activity. Multi-step metabolism creates tissue-specific conversion favoring epidermal effects. Identical downstream effects to tretinoin with reduced irritation.