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由于SRY核定位受损导致的人类性反转。临床相关性。

Human sex reversal due to impaired nuclear localization of SRY. A clinical correlation.

作者信息

Li B, Zhang W, Chan G, Jancso-Radek A, Liu S, Weiss M A

机构信息

Department of Biochemistry, Case Western Reserve University, School of Medicine, Cleveland, Ohio 44106, USA.

出版信息

J Biol Chem. 2001 Dec 7;276(49):46480-4. doi: 10.1074/jbc.C100388200.

Abstract

SRY, an architectural transcription factor encoded by the sex-determining region of the Y chromosome, initiates testicular differentiation in mammalian embryogenesis. The protein contains a high-mobility group (HMG) box, a DNA-bending motif conserved among a broad class of nuclear proteins. Mutations causing human sex reversal (46, XY pure gonadal dysgenesis) are clustered in this domain. Basic N- and C-terminal regions of the HMG box are each proposed to provide nuclear localization signals. The significance of the C-terminal basic cluster (SRY residues 130-134) is uncertain, however, as its activity in cell culture varies with assay conditions. To test its importance, we have investigated a C-terminal sex-reversal mutation (R133W, position 78 of the HMG box). This de novo mutation impairs nuclear localization but not specific DNA binding or sharp DNA bending. Correlation between these properties and the phenotype of the patient suggests that nuclear localization of SRY is required for testicular differentiation and directed in part by the C-terminal basic cluster. To our knowledge, these results provide the first example of impaired organogenesis due to a nuclear localization signal mutation.

摘要

SRY是一种由Y染色体性别决定区域编码的结构转录因子,在哺乳动物胚胎发育过程中启动睾丸分化。该蛋白质包含一个高迁移率族(HMG)盒,这是一种在广泛的核蛋白中保守的DNA弯曲基序。导致人类性反转(46, XY单纯性腺发育不全)的突变聚集在该结构域。HMG盒的基本N端和C端区域各自被认为提供核定位信号。然而,C端碱性簇(SRY第130 - 134位残基)的意义尚不确定,因为其在细胞培养中的活性随检测条件而变化。为了测试其重要性,我们研究了一个C端性反转突变(R133W,HMG盒第78位)。这个新生突变损害核定位,但不影响特异性DNA结合或明显的DNA弯曲。这些特性与患者表型之间的相关性表明,SRY的核定位是睾丸分化所必需的,并且部分由C端碱性簇指导。据我们所知,这些结果提供了首个因核定位信号突变导致器官发生受损的例子。

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