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人类体细胞中可诱导的XIST依赖性X染色体失活是可逆的。

Inducible XIST-dependent X-chromosome inactivation in human somatic cells is reversible.

作者信息

Chow Jennifer C, Hall Lisa L, Baldry Sarah E L, Thorogood Nancy P, Lawrence Jeanne B, Brown Carolyn J

机构信息

Department of Medical Genetics, Molecular Epigenetics Group, University of British Columbia, 2350 Health Sciences Mall, Vancouver, BC, Canada.

出版信息

Proc Natl Acad Sci U S A. 2007 Jun 12;104(24):10104-9. doi: 10.1073/pnas.0610946104. Epub 2007 May 30.

Abstract

During embryogenesis, the XIST RNA is expressed from and localizes to one X chromosome in females and induces chromosome-wide silencing. Although many changes to inactive X heterochromatin are known, the functional relationships between different modifications are not well understood, and studies of the initiation of X-inactivation have been largely confined to mouse. We now present a model system for human XIST RNA function in which induction of an XIST cDNA in somatic cells results in localized XIST RNA and transcriptional silencing. Chromatin immunoprecipitation and immunohistochemistry shows that this silencing need only be accompanied by a subset of heterochromatic marks and that these can differ between integration sites. Surprisingly, silencing is XIST-dependent, remaining reversible over extended periods. Deletion analysis demonstrates that the first exon of human XIST is sufficient for both transcript localization and the induction of silencing and that, unlike the situation in mice, the conserved repeat region is essential for both functions. In addition to providing mechanistic insights into chromosome regulation and formation of facultative heterochromatin, this work provides a tractable model system for the study of chromosome silencing and suggests key differences from mouse embryonic X-inactivation.

摘要

在胚胎发生过程中,XIST RNA在雌性个体中从一条X染色体表达并定位于该染色体,诱导全染色体范围的沉默。尽管已知失活X异染色质有许多变化,但不同修饰之间的功能关系尚未完全了解,而且X染色体失活起始的研究主要局限于小鼠。我们现在提出了一个用于研究人类XIST RNA功能的模型系统,其中在体细胞中诱导XIST cDNA会导致局部XIST RNA和转录沉默。染色质免疫沉淀和免疫组织化学表明,这种沉默仅需伴随着一部分异染色质标记,而且这些标记在整合位点之间可能不同。令人惊讶的是,沉默依赖于XIST,在很长一段时间内仍然是可逆的。缺失分析表明,人类XIST的第一个外显子对于转录本定位和沉默诱导都是足够的,而且与小鼠的情况不同,保守重复区域对于这两种功能都是必不可少的。除了为染色体调控和兼性异染色质的形成提供机制性见解外,这项工作还为染色体沉默的研究提供了一个易于处理的模型系统,并揭示了与小鼠胚胎X染色体失活的关键差异。

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本文引用的文献

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