Alpha-MSH Tripeptide Analogs Activate the Melanocortin 1 Receptor and Reduce UV-induced DNA Damage in Human Melanocytes

Overview

Journal Pigment Cell Melanoma Res

Date 2009 Jun 30

PMID 19558415

Citations 41

Authors

Zalfa A Abdel-Malek

Andrew Ruwe

Renny Kavanagh-Starner

Ana Luisa Kadekaro

Viki Swope

Carrie Haskell-Luevano

Leonid Koikov

James J Knittel

Affiliations

Soon will be listed here.

Abstract

One skin cancer prevention strategy that we are developing is based on synthesizing and testing melanocortin analogs that reduce and repair DNA damage resulting from exposure to solar ultraviolet (UV) radiation, in addition to stimulating pigmentation. Previously, we reported the effects of tetrapeptide analogs of alpha-melanocortin (alpha-MSH) that were more potent and stable than the physiological alpha-MSH, and mimicked its photoprotective effects against UV-induced DNA damage in human melanocytes. Here, we report on a panel of tripeptide analogs consisting of a modified alpha-MSH core His(6)-d-Phe(7)-Arg(8), which contained different N-capping groups, C-terminal modifications, or arginine mimics. The most potent tripeptides in activating cAMP formation and tyrosinase of human melanocytes were three analogs with C-terminal modifications. The most effective C-terminal tripeptide mimicked alpha-MSH in reducing hydrogen peroxide generation and enhancing nucleotide excision repair following UV irradiation. The effects of these three analogs required functional MC1R, as they were absent in human melanocytes that expressed non-functional receptor. These results demonstrate activation of the MC1R by tripeptide melanocortin analogs. Designing small analogs for topical delivery should prove practical and efficacious for skin cancer prevention.

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