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KMID : 0370220140580010021
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Yakhak Hoeji
2014 Volume.58 No. 1 p.21 ~ p.27
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Effects of Potential Melanocortin-1 Receptor Antagonists on Cultured Normal Human Melanocytes
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Lee Sang-Hwa
Chang Yun-Hee
Lee Seol-Hoon
Lee Jeung-Hoon
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Abstract
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We have developed 8 peptide derivatives as potential MC1R antagonists and their inhibitory effects on ¥á-MSH induced cell growth in cultured normal human melanocytes (NHM) were investigated. From these experiments, the two most potent peptide derivatives, 5-phenylvaleric acid-(D)His-Arg-Trp-(Lys)6NH2 (P 6) and 5-phenylvaleric acid-(D)His-Arg-Trp-(Lys)9NH2 (P 7) were selected for further studies. In ¥á-MSH depleted NHM cells, we have found that the treatment with 1 ¥ìM of these two peptide derivatives, P 6 and P 7, inhibited the cell proliferation induced by the addition of 1 nM ¥á-MSH by 70% and 72%, respectively. In NHM cells without previous ¥á-MSH depletion, 1 ¥ìM treatment in the presence of 10 nM ¥á-MSH resulted in 70% (P 6) and 80% (P 7) decrease in cell growth and 64% (P 6) and 71% (P 7) reduction in melanin synthesis, respectively. The peptide derivatives P 6 and P 7 were proved to have no apparent cytotoxicity and inhibited the elevation of intracellular cAMP concentration triggered by ¥á-MSH. In conclusion, our data suggest that the peptide derivatives reported in this study, 5-phenylvaleric acid-(D)His-Arg-Trp-(Lys)6NH2 (P 6) and 5-phenylvaleric acid-(D)His-Arg-Trp-(Lys)9NH2 (P 7) strongly antagonize ¥á-MSH, inhibit cell proliferation and melanin synthesis, and lower the intracellular
cAMP concentration, hence have a promising potential as a novel skin lightening agent.
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KEYWORD
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melanocortin 1 receptor, melanogenesis, ¥á-melanocyte stimulating hormone, cyclic adenosine mono phosphate, melanocyte
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