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黑皮质素-1受体是人类皮肤色素沉着的关键调节因子。

The melanocortin-1 receptor is a key regulator of human cutaneous pigmentation.

作者信息

Abdel-Malek Z, Scott M C, Suzuki I, Tada A, Im S, Lamoreux L, Ito S, Barsh G, Hearing V J

机构信息

University of Cincinnati, Ohio, 45267-592, USA.

出版信息

Pigment Cell Res. 2000;13 Suppl 8:156-62. doi: 10.1034/j.1600-0749.13.s8.28.x.

Abstract

The cloning and characterization of the human melanocortin-1 receptor (MC1R) and the demonstration that normal human melanocytes respond to the melanocortins, alpha-melanocyte stimulating hormone (alpha-MSH) and adrenocorticotrophic hormone (ACTH), with increased proliferation and eumelanogenesis had put an end to a long-standing controversy about the role of melanocortins in regulating human cutaneous pigmentation. We have shown that alpha-MSH and ACTH bind the human MC1R with equal affinity, and are equipotent in their mitogenic and melanogenic effects on human melanocytes. We also showed that the activation of the MC1R is important for the melanogenic response of human melanocytes to ultraviolet radiation (UVR). The MC1R is also the principal mediator of the inhibitory effects of agouti signaling protein (ASP) on melanogenesis. Expression of the MC1R is subject to regulation by its own ligands alpha-MSH and ACTH, as well as by UVR and endothelin-1. Recent studies that we conducted on the expression of MC1R variants by human melanocytes and the implications of these variants on the function of the MC1R revealed the following. Human melanocytes homozygous for Arg160Trp mutation in the MC1R demonstrated a significantly reduced response to alpha-MSH. Also, this culture responded poorly to ASP and exhibited an exaggerated cytotoxic response to UVR. Another culture, which was homozygous for Val92Met mutation in the MC1R, demonstrated a normal response to alpha-MSH. Heterozygous mutations that are frequently expressed in various melanocyte cultures did not disrupt MC1R function. These results begin to elucidate the significance of MC1R variants in the function of the receptor. Our data emphasize the significance of a normally functioning MC1R in the response of melanocytes to melanocortins, ASP, and UVR.

摘要

人类促黑素皮质素-1受体(MC1R)的克隆与特性分析,以及正常人类黑素细胞对促黑素、α-黑素细胞刺激素(α-MSH)和促肾上腺皮质激素(ACTH)产生增殖增加和真黑素生成反应的证明,终结了关于促黑素在调节人类皮肤色素沉着中作用的长期争议。我们已经表明,α-MSH和ACTH以同等亲和力结合人类MC1R,并且在对人类黑素细胞的促有丝分裂和黑素生成作用方面具有同等效力。我们还表明,MC1R的激活对于人类黑素细胞对紫外线辐射(UVR)的黑素生成反应很重要。MC1R也是刺鼠信号蛋白(ASP)对黑素生成抑制作用的主要介质。MC1R的表达受其自身配体α-MSH和ACTH以及UVR和内皮素-1的调节。我们最近对人类黑素细胞中MC1R变体的表达及其对MC1R功能的影响进行的研究揭示了以下内容。MC1R中Arg160Trp突变纯合的人类黑素细胞对α-MSH的反应明显降低。此外,这种培养物对ASP反应不佳,并且对UVR表现出过度的细胞毒性反应。另一种培养物,其MC1R中Val92Met突变纯合,对α-MSH表现出正常反应。在各种黑素细胞培养物中频繁表达的杂合突变并未破坏MC1R功能。这些结果开始阐明MC1R变体在受体功能中的意义。我们的数据强调了正常功能的MC1R在黑素细胞对促黑素、ASP和UVR反应中的重要性。

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