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MC1R Peptide Agonist Self-Assembles into a Hydrogel That Promotes Skin Pigmentation for Treating Vitiligo

Ci Zhu, Tingting Li, Zhuole Wang, Zenghui Li, Jiaying Wei, Hong Han, Dan Yuan, Minying Cai, Junfeng Shi

2023ACS Nano28 citationsDOI

Abstract

Vitiligo, a common skin disease that seriously affects 0.5-2.0% of the worldwide population, lacks approved therapeutics due to a wide range of adverse side effects. As a key regulator of skin pigmentation, MC1R may be an effective therapeutic target for vitiligo. Herein, we report an MC1R peptide agonist that directly self-assembles into nanofibrils that form a hydrogel matrix under normal physiological conditions. This hydrogel exhibits higher stability than free peptides, sustained release, rapid recovery from shear-thinning, and resistance to enzymatic proteolysis. Furthermore, this peptidal MC1R agonist upregulates tyrosinase, tyrosinase-related protein-1 (TYRP-1), and tyrosinase-related protein-2 (TYRP-2) to stimulate melanin synthesis. More importantly, MC1R agonist hydrogel promotes skin pigmentation in mice more potently than free MC1R agonist. This study supports the development of this MC1R agonist hydrogel as a promising pharmacological intervention for vitiligo.

Topics & Concepts

VitiligoAgonistTyrosinaseMelanocortin 1 receptorMelaninSelf-healing hydrogelsPeptideMelanocyteChemistryMedicineBiochemistryReceptorImmunologyCancer researchMelanomaEnzymeOrganic chemistryGeneAllelemelanin and skin pigmentationPhotochromic and Fluorescence ChemistrySupramolecular Self-Assembly in Materials
MC1R Peptide Agonist Self-Assembles into a Hydrogel That Promotes Skin Pigmentation for Treating Vitiligo | Litcius