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人类变异组蛋白基因的生长调控及编码蛋白的乙酰化作用

Growth regulation of human variant histone genes and acetylation of the encoded proteins.

作者信息

Alvelo-Ceron D, Niu L, Collart D G

机构信息

Department of Biological Sciences, Clark Atlanta University, GA 30314, USA.

出版信息

Mol Biol Rep. 2000 Jun;27(2):61-71. doi: 10.1023/a:1007156629024.

DOI:10.1023/a:1007156629024
PMID:11092552
Abstract

The family of human histone genes consists of replication-dependent and independent subtypes. The replication-independent histone genes, also known as variants, give rise to distinct mRNAs, whose expression is regulated depending on the growth state of the cell, tissue type and developmental stage. In turn, the histone variants are differentially synthesized and modified by acetylation. Consequently, chromatin structure is altered resulting in complex changes in gene expression. The high conservation among histone protein subtypes suggests that they are indispensable. In addition, conservation of the positions of acetylation within subtypes suggests that the location of these sites is functionally important for the eukaryotic cell. For example, the structures of transcriptionally active and repressed chromatin are different depending on the acetylation state of histone proteins [1-3]. In addition, transcriptionally active and repressed chromatin contains distinct histone variants [4]. Specialized histone variants are targeted to the centromere of the chromosome, where they are essential for chromosome segregation [5]. Other specialized histones exist that are essential for development [6]. Changes in histone acetylation have been implicated in the down-regulation of a tumour suppressor gene in human breast cancer [7]. Acetylation also plays an important role in X chromosome inactivation as well as hormone-mediated transcriptional regulation [8, 9]. We propose here a novel model for histone variant gene regulation at the post-transcriptional level, which provides the groundwork to define the pathways regulating the synthesis of these variants.

摘要

人类组蛋白基因家族由复制依赖型和复制非依赖型亚型组成。复制非依赖型组蛋白基因,也被称为变体,可产生不同的信使核糖核酸(mRNA),其表达根据细胞的生长状态、组织类型和发育阶段进行调控。反过来,组蛋白变体通过乙酰化进行差异合成和修饰。因此,染色质结构发生改变,导致基因表达出现复杂变化。组蛋白蛋白质亚型之间的高度保守性表明它们是不可或缺的。此外,亚型内乙酰化位置的保守性表明这些位点的位置对真核细胞具有重要功能。例如,转录活性染色质和抑制性染色质的结构因组蛋白的乙酰化状态而异[1 - 3]。此外,转录活性染色质和抑制性染色质含有不同的组蛋白变体[4]。特殊的组蛋白变体靶向染色体的着丝粒,在那里它们对染色体分离至关重要[5]。还存在其他对发育至关重要的确特殊组蛋白[6]。组蛋白乙酰化的变化与人类乳腺癌中肿瘤抑制基因的下调有关[7]。乙酰化在X染色体失活以及激素介导的转录调控中也起着重要作用[8, 9]。我们在此提出一种转录后水平上组蛋白变体基因调控的新模型,该模型为定义调控这些变体合成的途径奠定了基础。

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本文引用的文献

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ACETYLATION AND METHYLATION OF HISTONES AND THEIR POSSIBLE ROLE IN THE REGULATION OF RNA SYNTHESIS.组蛋白的乙酰化和甲基化及其在RNA合成调控中的可能作用。
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Acetylated histones are associated with FMR1 in normal but not fragile X-syndrome cells.在正常细胞而非脆性X综合征细胞中,乙酰化组蛋白与FMR1相关联。
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Esa1p is an essential histone acetyltransferase required for cell cycle progression.Esa1p是细胞周期进程所必需的一种组蛋白乙酰转移酶。
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The human H2A and H2B histone gene complement.人类H2A和H2B组蛋白基因复合体。
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Overlapping but distinct patterns of histone acetylation by the human coactivators p300 and PCAF within nucleosomal substrates.人类共激活因子p300和PCAF在核小体底物上的组蛋白乙酰化模式相互重叠但又有所不同。
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