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ATRX标记体细胞中的失活X染色体(Xi)以及滋养层干细胞中印记X染色体失活过程中的失活X染色体。

ATRX marks the inactive X chromosome (Xi) in somatic cells and during imprinted X chromosome inactivation in trophoblast stem cells.

作者信息

Baumann Claudia, De La Fuente Rabindranath

机构信息

Department of Clinical Studies, Center for Animal Transgenesis and Germ Cell Research, University of Pennsylvania, New Bolton Center, Kennett Square, PA, 19348, USA.

出版信息

Chromosoma. 2009 Apr;118(2):209-22. doi: 10.1007/s00412-008-0189-x. Epub 2008 Nov 13.

Abstract

Mammalian X chromosome inactivation (XCI) is an essential mechanism to compensate for dosage imbalances between male and female embryos. Although the molecular pathways are not fully understood, heterochromatinization of the Xi requires the coordinate recruitment of multiple epigenetic marks. Using fluorescence in situ hybridization analysis combined with immunocytochemistry, we demonstrate that the chromatin remodeling protein ATRX decorates the chromatids of a single, late replicating X chromosome in female somatic cells and co-localizes with the bona fide marker of the Xi, macroH2A1.2. Chromatin immunoprecipitation using somatic, embryonic stem (ES) cells and trophoblast stem (TS) cells as model for random and imprinted XCI, respectively, revealed that, in somatic and TS cells, ATRX exhibits a specific association with sequences located within the previously described H3K9me2-hotspot, a region 5' to the X inactive-specific transcript (Xist) locus. While no ATRX-Xi interaction was detectable in undifferentiated ES cells, an enrichment of ATRX was observed after 8 days of differentiation, indicating that ATRX associates with the Xi following the onset of random XCI, consistent with a potential role in maintenance of XCI. These results have important implications regarding a previously described escape from imprinted XCI in ATRX-deficient mice as well as cases of skewed XCI in patients with ATRX syndrome.

摘要

哺乳动物X染色体失活(XCI)是一种补偿雄性和雌性胚胎之间剂量失衡的重要机制。尽管分子途径尚未完全了解,但Xi的异染色质化需要多种表观遗传标记的协同募集。通过结合免疫细胞化学的荧光原位杂交分析,我们证明染色质重塑蛋白ATRX在雌性体细胞中修饰单个晚期复制X染色体的染色单体,并与Xi的真正标记macroH2A1.2共定位。分别使用体细胞、胚胎干细胞(ES)和滋养层干细胞(TS)作为随机和印记XCI模型的染色质免疫沉淀显示,在体细胞和TS细胞中,ATRX与位于先前描述的H3K9me2热点(Xist基因座5'端的一个区域)内的序列表现出特异性关联。虽然在未分化的ES细胞中未检测到ATRX与Xi的相互作用,但在分化8天后观察到ATRX富集,表明ATRX在随机XCI开始后与Xi相关联,这与它在维持XCI中的潜在作用一致。这些结果对于先前描述的ATRX缺陷小鼠中印记XCI的逃逸以及ATRX综合征患者中XCI偏斜的情况具有重要意义。

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