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银色基因座产物Pmel17/gp100/Silv/ME20:名称和功能均存在争议。

The Silver locus product Pmel17/gp100/Silv/ME20: controversial in name and in function.

作者信息

Theos Alexander C, Truschel Steven T, Raposo Graça, Marks Michael S

机构信息

Department of Pathology and Laboratory Medicine, University of Pennsylvania, Philadelphia, PA, USA.

出版信息

Pigment Cell Res. 2005 Oct;18(5):322-36. doi: 10.1111/j.1600-0749.2005.00269.x.

Abstract

Mouse coat color mutants have led to the identification of more than 120 genes that encode proteins involved in all aspects of pigmentation, from the regulation of melanocyte development and differentiation to the transcriptional activation of pigment genes, from the enzymatic formation of pigment to the control of melanosome biogenesis and movement [Bennett and Lamoreux (2003) Pigment Cell Res. 16, 333]. One of the more perplexing of the identified mouse pigment genes is encoded at the Silver locus, first identified by Dunn and Thigpen [(1930) J. Heredity 21, 495] as responsible for a recessive coat color dilution that worsened with age on black backgrounds. The product of the Silver gene has since been discovered numerous times in different contexts, including the initial search for the tyrosinase gene, the characterization of major melanosome constituents in various species, and the identification of tumor-associated antigens from melanoma patients. Each discoverer provided a distinct name: Pmel17, gp100, gp95, gp85, ME20, RPE1, SILV and MMP115 among others. Although all its functions are unlikely to have yet been fully described, the protein clearly plays a central role in the biogenesis of the early stages of the pigment organelle, the melanosome, in birds, and mammals. As such, we will refer to the protein in this review simply as pre-melanosomal protein (Pmel). This review will summarize the structural and functional aspects of Pmel and its role in melanosome biogenesis.

摘要

小鼠毛色突变体已促使人们鉴定出120多个基因,这些基因编码的蛋白质参与色素沉着的各个方面,从黑素细胞的发育和分化调控到色素基因的转录激活,从色素的酶促形成到黑素小体生物发生和移动的控制[贝内特和拉莫勒克斯(2003年)《色素细胞研究》16卷,第333页]。已鉴定出的小鼠色素基因中,较令人困惑的一个基因位于银色位点,该位点最早由邓恩和西格彭[(1930年)《遗传学期刊》21卷,第495页]鉴定,它导致隐性毛色变淡,并在黑色背景下随年龄增长而加重。此后,银色基因的产物在不同背景下被多次发现,包括最初对酪氨酸酶基因的搜索、各种物种中主要黑素小体成分的表征,以及黑色素瘤患者肿瘤相关抗原的鉴定。每个发现者都给出了一个不同的名称:Pmel17、gp100、gp95、gp85、ME20、RPE1、SILV和MMP115等。尽管其所有功能可能尚未完全描述清楚,但该蛋白质显然在鸟类和哺乳动物色素细胞器黑素小体早期生物发生中起着核心作用。因此,在本综述中,我们将该蛋白质简称为黑素小体前体蛋白(Pmel)。本综述将总结Pmel的结构和功能方面及其在黑素小体生物发生中的作用。

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