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Insights on the regulation of the MLL/SET1 family histone methyltransferases

机译:关于调节MLL / SET1家族组甲基转移酶的洞察

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In eukaryotes, histone H3K4 methylation by the MLL/SET1 family histone methyltransferases is enriched at transcription regulatory elements including gene promoters and enhancers. The level of H3K4 methylation is highly correlated with transcription activation and is one of the most frequently used histone post-translational modifications to predict transcriptional outcome. Recently, it has been shown that rearrangement of the cellular landscape of H3K4 mono-methylation at distal enhancers precedes cell fate transition and is used for identification of novel regulatory elements for development and disease progression. Similarly, broad H3K4 tri-methylation regions have also been used to predict intrinsic tumor suppression properties of regulator regions in a variety of cellular models. Understanding the regulation for how H3K4 methylation is deposited and regulated is of paramount importance. In this review, we will discuss new findings on how the MLL/SET1 family enzymes are regulated on chromatin and their potential functional and regulatory implications. This article is part of a Special Issue entitled: The MLL family of proteins in normal development and disease edited by Thomas A Milne.
机译:在真核生物中,MLL / SET1家族组甲基转移酶的组蛋白H3K4甲基化在包括基因启动子和增强子的转录调节元件中富集。 H3K4甲基化水平与转录激活高度相关,并且是预测转录结果的最常使用的组蛋白的翻译后修饰之一。最近,已经表明,在远端增强剂处的H3K4单甲基化细胞景观的重排在细胞命运过渡之前,用于鉴定开发和疾病进展的新型调节因素。类似地,宽的H3K4三甲基化区域也已被用于预测各种细胞模型中调节区的内在肿瘤抑制性能。了解沉积和调节H3K4甲基化的调节是至关重要的。在本次审查中,我们将讨论如何对染色质调节MLL / Set1家族酶的新发现及其潜在的功能和监管影响。本文是题为特殊问题的一部分:托马斯一家Milne编辑的正常发育和疾病中的MLL系列蛋白质。

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