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The 14th Datta Lecture. TFIIH: from transcription to clinic. 总被引:1,自引:0,他引:1
J M Egly 《FEBS letters》2001,498(2-3):124-128
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Busso D Keriel A Sandrock B Poterszman A Gileadi O Egly JM 《The Journal of biological chemistry》2000,275(30):22815-22823
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Jawhari A Lainé JP Dubaele S Lamour V Poterszman A Coin F Moras D Egly JM 《The Journal of biological chemistry》2002,277(35):31761-31767
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Molecular structure of human TFIIH 总被引:8,自引:0,他引:8
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Valentyn Oksenych Bruno Bernardes de Jesus Alexander Zhovmer Jean‐Marc Egly Frédéric Coin 《The EMBO journal》2009,28(19):2971-2980
XPB and XPD subunits of TFIIH are central genome caretakers involved in nucleotide excision repair (NER), although their respective role within this DNA repair pathway remains difficult to delineate. To obtain insight into the function of XPB and XPD, we studied cell lines expressing XPB or XPD ATPase‐deficient complexes. We show the involvement of XPB, but not XPD, in the accumulation of TFIIH to sites of DNA damage. Recruitment of TFIIH occurs independently of the helicase activity of XPB, but requires two recently identified motifs, a R‐E‐D residue loop and a Thumb‐like domain. Furthermore, we show that these motifs are specifically involved in the DNA‐induced stimulation of the ATPase activity of XPB. Together, our data demonstrate that the recruitment of TFIIH to sites of damage is an active process, under the control of the ATPase motifs of XPB and suggest that this subunit functions as an ATP‐driven hook to stabilize the binding of the TFIIH to damaged DNA. 相似文献
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