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A chromatin remodeling factor, BRM has important roles in cell differentiation

机译:染色质改造因子,BRM在细胞分化中具有重要作用

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The modification of chromatin structure is increasingly recognized to be an important factor for transcriptional regulation. So far, it is known that the state of chromatin compaction is controlled by two major mechanisms. One is a histone acetyltransferase and deacetylase system and the other is a regulatory system containing chromatin remodeling complexes. The former enzymes acetylate or deacetylate N-terminal tail structures of histones and control chromatin opening and compaction. The chromatinremodeling complex was characterized first in Saccharo/nyces cerevisiae as a multi-protein complex which controls mating type switch (SWI) and sucrose non-fermenting (SNF) genes. ATP-dependent chromatin remodeling activity of the complex was recently identified. This SWI/SNF complex has an ATPase subunit called SWI2/SNF2, and its activity is essential for chromatin remodeling. The homologs of SWI2/SNF2 have heen identified in higher eukaryotes, and they also form multi-protein complexes of chromatin remodeling factors. Mammalian SWI/SNF complexes are composed of more than 8 subunits. Until now, two ATPase subunits have been identified and named BRM and BRG1. The SWI/SNF complex containing either BRG1 or BRM shows chromatin remodeling activity, and activates or inactivates gene expression. In this article, we analyzed BRM and BRG1 expression during neural differentiation of NPCs and P19 embryonal carcinoma cells and liver differentiation to study its role in neural differentiation.
机译:染色质结构的改性越来越被认为是转录调控的重要因素。到目前为止,已知染色质压实的状态由两个主要机制控制。一种是组蛋白乙酰转移酶和脱乙酰酶系统,另一个是含有染色质重塑复合物的调节系统。原酶乙酰化物或脱乙酰酯N-末端尾部尾部结构和对照染色质开口和压实。染色体肾上腺素复合物的特征在于Saccharo / Nyces Cerevisiae作为多蛋白质复合物,其控制配合型开关(SWI)和蔗糖非发酵(SNF)基因。最近鉴定了复合物的ATP依赖性染色质重塑活性。该SWI / SNF复合物具有叫做SWI2 / SNF2的ATP酶亚基,其活性对于染色质重塑至关重要。 SWI2 / SNF2的同源物在较高的真核生物中鉴定了HEEEN,并且它们还形成染色质重塑因子的多蛋白质复合物。哺乳动物SWI / SNF复合物由超过8个亚基组成。到目前为止,已识别出两个ATP杂志亚基并命名为BRM和BRG1。含有BRG1或BRM的SWI / SNF络合物显示染色质改造活性,并激活或灭活基因表达。在本文中,我们在NPC和P19胚胎癌细胞的神经分化期间分析了BRM和BRG1表达,肝脏分化研究其在神经分化中的作用。

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