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SNF2β-BRG1对F9小鼠胚胎癌细胞的生存能力至关重要。

SNF2beta-BRG1 is essential for the viability of F9 murine embryonal carcinoma cells.

作者信息

Sumi-Ichinose C, Ichinose H, Metzger D, Chambon P

机构信息

Institut de Génétique et de Biologie Moléculaire et Cellulaire, CNRS/INSERM/ULP, Collège de France, Illkirch, CU de Strasbourg.

出版信息

Mol Cell Biol. 1997 Oct;17(10):5976-86. doi: 10.1128/MCB.17.10.5976.

Abstract

The yeast and animal SNF-SWI and related multiprotein complexes are thought to play an important role in processes, such as transcription factor binding to regulatory elements, which require nucleosome remodeling in order to relieve the repressing effect of packaging DNA in chromatin. There are two mammalian homologs of the yeast SNF2-SWI2 subunit protein, SNF2alpha-brm and SNF2beta-BRG1, and overexpression of either one of them has been shown to enhance transcriptional activation by glucocorticoid, estrogen, and retinoic acid (RA) receptors in transiently transfected cells. We have investigated here the function of SNF2beta-BRG1 in the RA receptor-retinoid X receptor-mediated transduction of the retinoid signal in F9 embryonal carcinoma (EC) cells which differentiate into endodermal-like cells upon RA treatment. The two SNF2beta-BRG1 alleles have been targeted by homologous recombination and subsequently disrupted by using a conditional Cre recombinase. We show that F9 EC cells inactivated on both SNF2beta alleles are not viable and that heterozygous mutant cells are affected in proliferation but not in RA-induced differentiation. Thus, in F9 EC cells, SNF2beta-BRG1 appears to play an essential role in basal processes involved in cell proliferation, in addition to its putative role in the activation of transcription mediated by nuclear receptors.

摘要

酵母和动物的SNF-SWI及相关多蛋白复合物被认为在转录因子与调控元件结合等过程中发挥重要作用,这些过程需要核小体重塑以解除染色质中DNA包装的抑制作用。酵母SNF2-SWI2亚基蛋白有两个哺乳动物同源物,即SNF2α-brm和SNF2β-BRG1,在瞬时转染细胞中,其中任何一个的过表达都已显示可增强糖皮质激素、雌激素和视黄酸(RA)受体介导的转录激活。我们在此研究了SNF2β-BRG1在F9胚胎癌细胞中RA受体-视黄酸X受体介导的类视黄醇信号转导中的功能,F9胚胎癌细胞在RA处理后可分化为内胚层样细胞。通过同源重组靶向了两个SNF2β-BRG1等位基因,随后使用条件性Cre重组酶将其破坏。我们发现,两个SNF2β等位基因均失活的F9胚胎癌细胞无法存活,杂合突变细胞的增殖受到影响,但RA诱导的分化未受影响。因此,在F9胚胎癌细胞中,SNF2β-BRG1除了在核受体介导的转录激活中可能发挥的作用外,似乎在细胞增殖所涉及的基础过程中也起着至关重要的作用。

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