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通过结合SATB1和GATA-3的脱氧核糖核酸酶I超敏位点和基质附着区域的共定位,鉴定人类CD8基因复合体中的一个候选调控区域。

Identification of a candidate regulatory region in the human CD8 gene complex by colocalization of DNase I hypersensitive sites and matrix attachment regions which bind SATB1 and GATA-3.

作者信息

Kieffer Lynda J, Greally John M, Landres Inna, Nag Shanta, Nakajima Yuko, Kohwi-Shigematsu Terumi, Kavathas Paula B

机构信息

Department of Laboratory Medicine and Department of Genetics and Section of Immunobiology, Yale University, New Haven, CT 06520, USA.

出版信息

J Immunol. 2002 Apr 15;168(8):3915-22. doi: 10.4049/jimmunol.168.8.3915.

DOI:10.4049/jimmunol.168.8.3915
PMID:11937547
Abstract

To locate elements regulating the human CD8 gene complex, we mapped nuclear matrix attachment regions (MARs) and DNase I hypersensitive (HS) sites over a 100-kb region that included the CD8B gene, the intergenic region, and the CD8A gene. MARs facilitate long-range chromatin remodeling required for enhancer activity and have been found closely linked to several lymphoid enhancers. Within the human CD8 gene complex, we identified six DNase HS clusters, four strong MARs, and several weaker MARs. Three of the strong MARs were closely linked to two tissue-specific DNase HS clusters (III and IV) at the 3' end of the CD8B gene. To further establish the importance of this region, we obtained 19 kb of sequence and screened for potential binding sites for the MAR-binding protein, SATB1, and for GATA-3, both of which are critical for T cell development. By gel shift analysis we identified two strong SATB1 binding sites, located 4.5 kb apart, in strong MARs. We also detected strong GATA-3 binding to an oligonucleotide containing two GATA-3 motifs located at an HS site in cluster IV. This clustering of DNase HS sites and MARs capable of binding SATB1 and GATA-3 at the 3' end of the CD8B gene suggests that this region is an epigenetic regulator of CD8 expression.

摘要

为了定位调控人类CD8基因复合体的元件,我们在一个包含CD8B基因、基因间区域和CD8A基因的100 kb区域内绘制了核基质附着区域(MARs)和DNase I超敏(HS)位点。MARs促进增强子活性所需的长程染色质重塑,并且已发现其与多个淋巴样增强子紧密相连。在人类CD8基因复合体内,我们鉴定出六个DNase HS簇、四个强MARs和几个较弱的MARs。其中三个强MARs与CD8B基因3'端的两个组织特异性DNase HS簇(III和IV)紧密相连。为了进一步确定该区域的重要性,我们获得了19 kb的序列,并筛选了MAR结合蛋白SATB1和GATA-3的潜在结合位点,这两者对T细胞发育都至关重要。通过凝胶迁移分析,我们在强MARs中鉴定出两个相距4.5 kb的强SATB1结合位点。我们还检测到GATA-3与一个包含位于簇IV中一个HS位点的两个GATA-3基序的寡核苷酸有强结合。CD8B基因3'端的DNase HS位点和能够结合SATB1和GATA-3的MARs的这种聚集表明该区域是CD8表达的表观遗传调节因子。

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