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Med5(Nut1) and Med17(Srb4) Are Direct Targets of Mediator Histone H4 Tail Interactions

机译:Med5(Nut1)和Med17(Srb4)是介体Histone H4尾部相互作用的直接目标

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摘要

The Mediator complex transmits activation signals from DNA bound transcription factors to the core transcription machinery. In addition to its canonical role in transcriptional activation, recent studies have demonstrated that S. cerevisiae Mediator can interact directly with nucleosomes, and their histone tails. Mutations in Mediator subunits have shown that Mediator and certain chromatin structures mutually impact each other structurally and functionally in vivo. We have taken a UV photo cross-linking approach to further delineate the molecular basis of Mediator chromatin interactions and help determine whether the impact of certain Mediator mutants on chromatin is direct. Specifically, by using histone tail peptides substituted with an amino acid analog that is a UV activatible crosslinker, we have identified specific subunits within Mediator that participate in histone tail interactions. Using Mediator purified from mutant yeast strains we have evaluated the impact of these subunits on histone tail binding. This analysis has identified the Med5 subunit of Mediator as a target for histone tail interactions and suggests that the previously observed effect of med5 mutations on telomeric heterochromatin and silencing is direct.
机译:介体复合物将激活信号从DNA结合的转录因子传递到核心转录机制。除了其在转录激活中的典型作用外,最近的研究表明,酿酒酵母介体可以与核小体及其组蛋白尾巴直接相互作用。介体亚基的突变表明,介体和某些染色质结构在体内相互影响结构和功能。我们采用了紫外线照片交联方法来进一步描述介体染色质相互作用的分子基础,并帮助确定某些介体突变体对染色质的影响是否直接。具体来说,通过使用被氨基酸类似物(是紫外线可激活的交联剂)取代的组蛋白尾巴肽,我们已经确定了介体中参与组蛋白尾巴相互作用的特定亚基。使用从突变酵母菌株中纯化的介体,我们评估了这些亚基对组蛋白尾巴结合的影响。该分析已确定介体的Med5亚基为组蛋白尾巴相互作用的靶标,并表明先前观察到的med5突变对端粒异染色质和沉默的影响是直接的。

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