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免疫球蛋白重链基因座潜在3'端附近的染色质结构涉及B细胞发育过程中组蛋白修饰的模块化调控以及CTCF位点在体内的占据情况。

Chromatin architecture near a potential 3' end of the igh locus involves modular regulation of histone modifications during B-Cell development and in vivo occupancy at CTCF sites.

作者信息

Garrett Francine E, Emelyanov Alexander V, Sepulveda Manuel A, Flanagan Patrick, Volpi Sabrina, Li Fubin, Loukinov Dmitry, Eckhardt Laurel A, Lobanenkov Victor V, Birshtein Barbara K

机构信息

Albert Einstein College of Medicine, Department of Cell Biology, Bronx, NY 10461, USA.

出版信息

Mol Cell Biol. 2005 Feb;25(4):1511-25. doi: 10.1128/MCB.25.4.1511-1525.2005.

Abstract

The murine Igh locus has a 3' regulatory region (3' RR) containing four enhancers (hs3A, hs1,2, hs3B, and hs4) at DNase I-hypersensitive sites. The 3' RR exerts long-range effects on class switch recombination (CSR) to several isotypes through its control of germ line transcription. By measuring levels of acetylated histones H3 and H4 and of dimethylated H3 (K4) with chromatin immunoprecipitation assays, we found that early in B-cell development, chromatin encompassing the enhancers of the 3' RR began to attain stepwise modifications typical of an open conformation. The hs4 enhancer was associated with active chromatin initially in pro- and pre-B cells and then together with hs3A, hs1,2, and hs3B in B and plasma cells. Histone modifications were similar in resting splenic B cells and in splenic B cells induced by lipopolysaccharide to undergo CSR. From the pro-B-cell stage onward, the approximately 11-kb region immediately downstream of hs4 displayed H3 and H4 modifications indicative of open chromatin. This region contained newly identified DNase I-hypersensitive sites and several CTCF target sites, some of which were occupied in vivo in a developmentally regulated manner. The open chromatin environment of the extended 3' RR in mature B cells was flanked by regions associated with dimethylated K9 of histone H3. Together, these data suggest that 3' RR elements are located within a specific chromatin subdomain that contains CTCF binding sites and developmentally regulated modules.

摘要

小鼠免疫球蛋白重链(Igh)基因座有一个3'调控区(3'RR),在DNA酶I高敏位点含有四个增强子(hs3A、hs1,2、hs3B和hs4)。3'RR通过控制种系转录对向几种同种型的类别转换重组(CSR)发挥远程作用。通过染色质免疫沉淀分析测量组蛋白H3和H4的乙酰化水平以及H3(K4)的二甲基化水平,我们发现,在B细胞发育早期,包含3'RR增强子的染色质开始逐步获得开放构象特有的修饰。hs4增强子最初在原B细胞和前B细胞中与活性染色质相关,然后在B细胞和浆细胞中与hs3A、hs1,2和hs3B一起。静息脾B细胞和由脂多糖诱导进行CSR的脾B细胞中的组蛋白修饰相似。从原B细胞阶段开始,hs4下游紧邻的约11 kb区域显示出指示开放染色质的H3和H4修饰。该区域包含新鉴定的DNA酶I高敏位点和几个CTCF靶位点,其中一些在体内以发育调控的方式被占据。成熟B细胞中扩展的3'RR的开放染色质环境两侧是与组蛋白H3的K9二甲基化相关的区域。这些数据共同表明,3'RR元件位于一个特定的染色质亚结构域内,该亚结构域包含CTCF结合位点和发育调控模块。

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