Glycolic AcidvsNiacinamide

Glycolic acid disrupts ionic bonds between corneocytes (dead skin cells) in the stratum corneum by chelating calcium ions and lowering the calcium concentration at desmosomal junctions. This weakens corneodesmosome integrity and activates endogenous proteases (kallikrein 5 and 7), accelerating desquamation. At higher concentrations, glycolic acid penetrates the viable epidermis and dermis, where it stimulates keratinocyte differentiation and upregulates transforming growth factor-beta (TGF-β) signaling in fibroblasts. This promotes glycosaminoglycan (GAG) synthesis, type I and III collagen production via procollagen gene expression, and elastin remodeling. Its small molecular size (76 Da) and high water solubility give it the deepest penetration of any AHA. The exfoliation also improves barrier function over time by promoting proper corneocyte maturation and reducing stratum corneum compaction.

Niacinamide is converted to NAD+ via the Preiss-Handler pathway—essential for cellular respiration, DNA repair (PARP), and sirtuin regulation. In keratinocytes, it upregulates serine palmitoyltransferase and fatty acid elongases, increasing ceramide synthesis and strengthening the barrier. It inhibits melanosome transfer by downregulating protease-activated receptor-2 (PAR-2) on keratinocytes—brightening without tyrosinase inhibition. In sebocytes, it normalizes lipid synthesis and reduces sebum (possibly via AMPK). Niacinamide inhibits NF-kB translocation, suppressing IL-1beta, TNF-alpha, and IL-8. It inhibits phosphodiesterase, increasing cAMP and modulating keratinocyte differentiation. These multi-pathway effects explain broad efficacy across barrier repair, brightening, acne, and anti-aging.