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促黑素细胞激素和促黑素细胞激素1受体,在预防黑色素瘤方面取得进展。

Melanocortins and the melanocortin 1 receptor, moving translationally towards melanoma prevention.

作者信息

Abdel-Malek Zalfa A, Swope Viki B, Starner Renny J, Koikov Leonid, Cassidy Pamela, Leachman Sancy

机构信息

Department of Dermatology, University of Cincinnati, United States.

Department of Dermatology, University of Cincinnati, United States.

出版信息

Arch Biochem Biophys. 2014 Dec 1;563:4-12. doi: 10.1016/j.abb.2014.07.002. Epub 2014 Jul 11.

DOI:10.1016/j.abb.2014.07.002
PMID:25017567
Abstract

Beginning in the last decade of the twentieth century, the fields of pigment cell research and melanoma have witnessed major breakthroughs in the understanding of the role of melanocortins in human pigmentation and the DNA damage response of human melanocytes to solar ultraviolet radiation (UV). This began with the cloning of the melanocortin 1 receptor (MC1R) gene from human melanocytes and the demonstration that the encoded receptor is functional. Subsequently, population studies found that the MC1R gene is highly polymorphic, and that some of its variants are associated with red hair phenotype, fair skin and poor tanning ability. Using human melanocytes cultured from donors with different MC1R genotypes revealed that the alleles associated with red hair color encode for a non-functional receptor. Epidemiological studies linked the MC1R red hair color variants to increased melanoma risk. Investigating the impact of different MC1R variants on the response of human melanocytes to UV led to the important discovery that the MC1R signaling activates antioxidant, DNA repair and survival pathways, in addition to stimulation of eumelanin synthesis. These effects of MC1R were absent in melanocytes expressing 2 MC1R red hair color variants that result in loss of function of the receptor. The importance of the MC1R in reducing UV-induced genotoxicity in melanocytes led us to design small peptide analogs of the physiological MC1R agonist α-melanocortin (α-melanocyte stimulating hormone; α-MSH) for the goal of utilizing them for melanoma chemoprevention.

摘要

从二十世纪的最后十年开始,色素细胞研究和黑色素瘤领域在理解黑皮质素在人类色素沉着中的作用以及人类黑素细胞对太阳紫外线辐射(UV)的DNA损伤反应方面取得了重大突破。这始于从人类黑素细胞中克隆黑皮质素1受体(MC1R)基因,并证明所编码的受体具有功能。随后,群体研究发现MC1R基因具有高度多态性,其一些变体与红发表型、白皙皮肤和较差的晒黑能力相关。使用从具有不同MC1R基因型的供体培养的人类黑素细胞表明,与红发颜色相关的等位基因编码无功能的受体。流行病学研究将MC1R红发颜色变体与黑色素瘤风险增加联系起来。研究不同MC1R变体对人类黑素细胞对UV反应的影响导致了一个重要发现,即MC1R信号除了刺激真黑素合成外,还激活抗氧化、DNA修复和生存途径。在表达导致受体功能丧失的2种MC1R红发颜色变体的黑素细胞中,MC1R的这些作用不存在。MC1R在降低黑素细胞中UV诱导的遗传毒性方面的重要性促使我们设计生理性MC1R激动剂α-黑素细胞刺激素(α-MSH)的小肽类似物,目的是将它们用于黑色素瘤化学预防。

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