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SATB1靶向染色质重塑以远距离调控基因。

SATB1 targets chromatin remodelling to regulate genes over long distances.

作者信息

Yasui Dag, Miyano Masaru, Cai Shutao, Varga-Weisz Patrick, Kohwi-Shigematsu Terumi

机构信息

Life Sciences Division, Lawrence Berkeley National Laboratory, University of California, Berkeley 94720, USA.

出版信息

Nature. 2002 Oct 10;419(6907):641-5. doi: 10.1038/nature01084.

Abstract

Eukaryotic chromosomes are organized inside the nucleus in such a way that only a subset of the genome is expressed in any given cell type, but the details of this organization are largely unknown. SATB1 ('special AT-rich sequence binding 1'), a protein found predominantly in thymocytes, regulates genes by folding chromatin into loop domains, tethering specialized DNA elements to an SATB1 network structure. Ablation of SATB1 by gene targeting results in temporal and spatial mis-expression of numerous genes and arrested T-cell development, suggesting that SATB1 is a cell-type specific global gene regulator. Here we show that SATB1 targets chromatin remodelling to the IL-2Ralpha ('interleukin-2 receptor alpha') gene, which is ectopically transcribed in SATB1 null thymocytes. SATB1 recruits the histone deacetylase contained in the NURD chromatin remodelling complex to a SATB1-bound site in the IL-2Ralpha locus, and mediates the specific deacetylation of histones in a large domain within the locus. SATB1 also targets ACF1 and ISWI, subunits of CHRAC and ACF nucleosome mobilizing complexes, to this specific site and regulates nucleosome positioning over seven kilobases. SATB1 defines a class of transcriptional regulators that function as a 'landing platform' for several chromatin remodelling enzymes and hence regulate large chromatin domains.

摘要

真核生物的染色体在细胞核内以这样一种方式组织,即任何给定细胞类型中只有基因组的一个子集被表达,但这种组织的细节在很大程度上尚不清楚。SATB1(“富含AT的特殊序列结合蛋白1”)是一种主要在胸腺细胞中发现的蛋白质,它通过将染色质折叠成环结构域来调节基因,将特殊的DNA元件拴系到SATB1网络结构上。通过基因靶向敲除SATB1会导致众多基因在时间和空间上的错误表达以及T细胞发育停滞,这表明SATB1是一种细胞类型特异性的全局基因调节因子。在这里,我们表明SATB1将染色质重塑靶向到IL-2Rα(“白细胞介素-2受体α”)基因,该基因在SATB1缺失的胸腺细胞中异位转录。SATB1将包含在NURD染色质重塑复合物中的组蛋白去乙酰化酶招募到IL-2Rα基因座中与SATB1结合的位点,并介导该基因座内一个大区域内组蛋白的特异性去乙酰化。SATB1还将CHRAC和ACF核小体移动复合物的亚基ACF1和ISWI靶向到这个特定位点,并调节超过七千个碱基上的核小体定位。SATB1定义了一类转录调节因子,它们作为几种染色质重塑酶的“着陆平台”发挥作用,从而调节大的染色质结构域。

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