首页> 外文期刊>Nucleic Acids Research >Structural and functional evidence that Rad4 competes with Rad2 for binding to the Tfb1 subunit of TFIIH in NER
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Structural and functional evidence that Rad4 competes with Rad2 for binding to the Tfb1 subunit of TFIIH in NER

机译:Rad4与Rad2竞争与NER中TFIIH的Tfb1亚基结合的结构和功能证据

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XPC/Rad4 (human/yeast) recruits transcription faction IIH (TFIIH) to the nucleotide excision repair (NER) complex through interactions with its p62/ Tfb1 and XPB/Ssl2 subunits. TFIIH then recruits XPG/Rad2 through interactions with similar subunits and the two repair factors appear to be mutually exclusive within the NER complex. Here, we show that Rad4 binds the PH domain of the Tfb1 (TfblPH) with high affinity. Structural characterization of a Rad4-Tfb1PH complex demonstrates that the Rad4-bindinginterface is formed using a motif similar to one used by Rad2 to bind TfblPH. In vivo studies in yeast demonstrate that the N-terminal Tfb1-binding motif and C-terminal TFIIH-binding motif of Rad4 are both crucial for survival following exposure to UV irradiation. Together, these results support the hypothesis that XPG/Rad2 displaces XPC/Rad4 from the repair complex in part through interactions with the Tfb1/p62 subunit of TFIIH, The Rad4-Tfb1PH structure also provides detailed information regarding, not only the interplay of TFIIH recruitment to the NER, but also links the role of TFIIH in NER and transcription.
机译:XPC / Rad4(人类/酵母)通过其p62 / Tfb1和XPB / Ssl2亚基的相互作用将转录因子IIH(TFIIH)募集到核苷酸切除修复(NER)复合物中。 TFIIH然后通过与相似亚基的相互作用募集XPG / Rad2,并且这两种修复因子在NER复合物中似乎是互斥的。在这里,我们显示Rad4以高亲和力结合Tfb1(TfblPH)的PH域。 Rad4-Tfb1PH复合物的结构表征表明,使用与Rad2用来结合TfblPH的基序相似的基序形成Rad4-bindinginterface。酵母中的体内研究表明,Rad4的N末端Tfb1结合基序和C末端TFIIH结合基序对于暴露于紫外线照射后的存活都是至关重要的。在一起,这些结果支持了XPG / Rad2部分地通过与TFIIH的Tfb1 / p62亚基相互作用而从修复复合物中置换XPC / Rad4的假设。Rad4-Tfb1PH结构还提供了有关TFIIH募集相互作用的详细信息不仅与NER相关,而且还与TFIIH在NER和转录中的作用有关。

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