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Histone acetylation: truth of consequences?

机译:组蛋白乙酰化:后果的真相?

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Eukaryotic DNA is packaged into a nucleoprotein structure known as chromatin, which is comprised of DNA, histones, and nonhistone proteins. Chromatin structure is highly dynamic, and can shift from a transcriptionally inactive state to an active form in response to intra- and extracellular signals. A major factor in chromatin architecture is the covalent modification of histones through the addition of chemical moieties, such as acetyl, methyl, ubiquitin, and phosphate groups. The acetylation of the amino-terminal tails of histones is a process that is highly conserved in eukaryotes, and was one of the earliest histone modifications characterized. Since its identification in 1964, a large body of evidence has accumulated demonstrating that histone acetylation plays an important role in transcription. Despite our ever-growing understanding of the nuclear processes involved in nucleosome acetylation, however, the exact biochemical mechanisms underlying the downstream effects of histone acetylation have yet to be fully elucidated. To date, histone acetylation has been proposed to function in 2 nonmutually exclusive manners: by directly altering chromatin structure, and by acting as a molecular tag for the recruitment of chromatin-modifying complexes. Here, we discuss recent research focusing on these 2 potential roles of histone acetylation and clarify what we actually know about the function of this modification.
机译:真核DNA被包装成核蛋白结构,即染色质,该结构由DNA,组蛋白和非组蛋白组成。染色质结构是高度动态的,并且可以响应于细胞内和细胞外信号而从转录无活性状态转变为活性形式。染色质结构的主要因素是通过添加化学部分(例如乙酰基,甲基,泛素和磷酸基)对组蛋白进行共价修饰。组蛋白氨基末端尾巴的乙酰化是在真核生物中高度保守的过程,并且是最早表征的组蛋白修饰之一。自从1964年鉴定以来,大量的证据表明,组蛋白乙酰化在转录中起着重要的作用。尽管我们对核小体乙酰化涉及的核过程的理解日益增长,但是,尚未完全阐明组蛋白乙酰化下游效应的确切生化机制。迄今为止,已提出组蛋白乙酰化以两种非互斥方式起作用:通过直接改变染色质结构,以及通过作为分子标签来募集染色质修饰复合物。在这里,我们讨论了针对组蛋白乙酰化这两个潜在作用的最新研究,并阐明了我们对这种修饰功能的实际了解。

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