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部分折叠的高危型人乳头瘤病毒45癌蛋白E7的溶液结构

Solution structure of the partially folded high-risk human papilloma virus 45 oncoprotein E7.

作者信息

Ohlenschläger O, Seiboth T, Zengerling H, Briese L, Marchanka A, Ramachandran R, Baum M, Korbas M, Meyer-Klaucke W, Dürst M, Görlach M

机构信息

Fritz-Lipmann-Institut, Jena, Germany.

出版信息

Oncogene. 2006 Sep 28;25(44):5953-9. doi: 10.1038/sj.onc.1209584. Epub 2006 Apr 24.

Abstract

The oncoprotein E7 of human papilloma viruses (HPV) is involved in the pathogenesis and maintenance of human cervical cancers. The most prevalent HPV types found in cervix carcinomas are HPV16, 18 and 45. The structure of the E7 dimer from HPV45 (PDB 2F8B) was determined by nuclear magnetic resonance spectroscopy. Each monomer comprises an unfolded N-terminus and a well-structured C-terminal domain with a beta1beta2alpha1beta3alpha2 topology representing a unique zinc-binding fold found only for E7. Dimerization occurs through the alpha1/alpha1' helices and intermolecular beta-sheet formation but excludes the zinc-binding sites. E7 is reported to interact with a number of cellular proteins (e.g. pRb, p21(CIP1)). Binding of a peptide derived from the C-terminus of p21(CIP1) to the C-terminal domain of E7 was characterized by monitoring chemical shift perturbations of the amide groups of E7. This provides direct evidence that a shallow groove situated between alpha1 and beta1 of the E7 C-terminal domain is interacting with the C-terminus of p21(CIP1). Intriguingly, this binding site overlaps with the low-affinity binding site on E7 for the C-domain of pRb.

摘要

人乳头瘤病毒(HPV)的癌蛋白E7参与人类宫颈癌的发病机制及维持过程。宫颈癌中最常见的HPV类型是HPV16、18和45。通过核磁共振光谱法确定了HPV45的E7二聚体结构(蛋白质数据银行编号2F8B)。每个单体包含一个未折叠的N端和一个结构良好的C端结构域,其具有β1β2α1β3α2拓扑结构,代表仅在E7中发现的独特锌结合折叠。二聚化通过α1/α1'螺旋和分子间β-折叠形成,但不包括锌结合位点。据报道,E7与多种细胞蛋白相互作用(例如pRb、p21(CIP1))。通过监测E7酰胺基团的化学位移扰动,对源自p21(CIP1)C端的肽与E7 C端结构域的结合进行了表征。这提供了直接证据,表明E7 C端结构域α1和β1之间的浅沟与p21(CIP1)的C端相互作用。有趣的是,该结合位点与E7上pRb C结构域的低亲和力结合位点重叠。

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