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XY性反转中Y染色体性别决定区域(SRY)的钙调蛋白介导的核转运缺陷。

Defective calmodulin-mediated nuclear transport of the sex-determining region of the Y chromosome (SRY) in XY sex reversal.

作者信息

Sim Helena, Rimmer Kieran, Kelly Sabine, Ludbrook Louisa M, Clayton Andrew H A, Harley Vincent R

机构信息

Prince Henry's Institute of Medical Research, Level 4 Block E, Monash Medical Centre, 246 Clayton Road, Clayton, Victoria 3168, Australia.

出版信息

Mol Endocrinol. 2005 Jul;19(7):1884-92. doi: 10.1210/me.2004-0334. Epub 2005 Mar 3.

DOI:10.1210/me.2004-0334
PMID:15746192
Abstract

The sex-determining region of the Y chromosome (SRY) plays a key role in human sex determination, as mutations in SRY can cause XY sex reversal. Although some SRY missense mutations affect DNA binding and bending activities, it is unclear how others contribute to disease. The high mobility group domain of SRY has two nuclear localization signals (NLS). Sex-reversing mutations in the NLSs affect nuclear import in some patients, associated with defective importin-beta binding to the C-terminal NLS (c-NLS), whereas in others, importin-beta recognition is normal, suggesting the existence of an importin-beta-independent nuclear import pathway. The SRY N-terminal NLS (n-NLS) binds calmodulin (CaM) in vitro, and here we show that this protein interaction is reduced in vivo by calmidazolium, a CaM antagonist. In calmidazolium-treated cells, the dramatic reduction in nuclear entry of SRY and an SRY-c-NLS mutant was not observed for two SRY-n-NLS mutants. Fluorescence spectroscopy studies reveal an unusual conformation of SRY.CaM complexes formed by the two n-NLS mutants. Thus, CaM may be involved directly in SRY nuclear import during gonadal development, and disruption of SRY.CaM recognition could underlie XY sex reversal. Given that the CaM-binding region of SRY is well-conserved among high mobility group box proteins, CaM-dependent nuclear import may underlie additional disease states.

摘要

Y染色体性别决定区(SRY)在人类性别决定中起关键作用,因为SRY的突变可导致XY性反转。尽管一些SRY错义突变会影响DNA结合和弯曲活性,但尚不清楚其他突变如何导致疾病。SRY的高迁移率族结构域有两个核定位信号(NLS)。NLS中的性别反转突变在一些患者中影响核输入,这与输入蛋白β与C端NLS(c-NLS)的结合缺陷有关,而在其他患者中,输入蛋白β的识别是正常的,这表明存在一条不依赖于输入蛋白β的核输入途径。SRY的N端NLS(n-NLS)在体外与钙调蛋白(CaM)结合,我们在此表明,钙调蛋白拮抗剂氯丙咪嗪在体内会减少这种蛋白质相互作用。在经氯丙咪嗪处理的细胞中,对于两个SRY-n-NLS突变体,未观察到SRY和SRY-c-NLS突变体的核进入显著减少。荧光光谱研究揭示了由两个n-NLS突变体形成的SRY·CaM复合物的异常构象。因此,CaM可能直接参与性腺发育过程中的SRY核输入,而SRY·CaM识别的破坏可能是XY性反转的基础。鉴于SRY的CaM结合区域在高迁移率族框蛋白中高度保守,CaM依赖性核输入可能是其他疾病状态的基础。

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