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首页> 外文期刊>Epigenetics: official journal of the DNA Methylation Society >An essential interaction between T-box proteins and histone-modifying enzymes.
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An essential interaction between T-box proteins and histone-modifying enzymes.

机译:T-box蛋白与组蛋白修饰酶之间的基本相互作用。

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摘要

Cellular differentiation requires precisely coordinated events to induce developmentally appropriate gene expression profiles. Lineage-defining transcription factors are responsible for establishing cell-type specific gene expression patterns during development. Recently, we reported a novel mechanism by which the T-box transcription factor T-bet interacts with JMJD3, an H3K27-demethylase, and Set7/9, an H3K4-methyltransferase (Genes Dev. 2008. 22: 2980-2993). Importantly, separable contact points in the T-box DNA binding domain mediate these interactions. Due to the highly conserved nature of the contact residues, these represent common interactions for the T-box family. Therefore, studies examining the molecular mechanisms that account for the ability of T-bet to regulate Ifng and Cxcr3, prototypic CD4+ Th1 genes, have provided novel insight into essential regulatory events that occur at diverse developmental transitions. In this article, we discuss the implications for these findings as well as explore the role epigenetic mechanisms may play in the development of human genetic diseases that are caused by T-box mutations, including congenital heart defects, cleft palate, pituitary deficiencies, and Ulnar-mammary syndrome.
机译:细胞分化需要精确协调的事件来诱导发育上适当的基因表达谱。谱系定义转录因子负责在发育过程中建立细胞类型的特定基因表达模式。最近,我们报道了一种新的机制,通过该机制,T盒转录因子T-bet与JMJD3(一种H3K27-脱甲基酶)和Set7 / 9(一种H3K4-甲基转移酶)相互作用(Genes Dev。2008. 22:2980-2993)。重要的是,T-box DNA结合域中的可分离接触点介导了这些相互作用。由于接触残基的高度保守性质,它们代表了T-box家族的常见相互作用。因此,研究分子机制解释了T-bet调节Ifng和原型CD4 + Th1基因Cxcr3的能力的分子机制,为在各种发育过渡中发生的基本调控事件提供了新的见解。在本文中,我们讨论了这些发现的意义,并探讨了表观遗传机制在由T型盒突变引起的人类遗传疾病的发展中可能发挥的作用,这些突变包括先天性心脏病,c裂,垂体功能低下和尺骨-乳腺综合症。

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