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Crystal structure of the SF3 helicase from adeno-associated virus type 2.2型腺相关病毒SF3解旋酶的晶体结构
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A biochemical characterization of the adeno-associated virus Rep40 helicase.腺相关病毒Rep40解旋酶的生化特性
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Structure of the replicative helicase of the oncoprotein SV40 large tumour antigen.致癌蛋白SV40大肿瘤抗原复制解旋酶的结构。
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RecQ helicases: caretakers of the genome.RecQ解旋酶:基因组守护者。
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ATP-mediated conformational changes in the RecA filament.ATP介导的RecA丝状体构象变化。
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9
Structural studies on MtRecA-nucleotide complexes: insights into DNA and nucleotide binding and the structural signature of NTP recognition.MtRecA-核苷酸复合物的结构研究:对DNA和核苷酸结合以及NTP识别的结构特征的深入了解。
Proteins. 2003 Feb 15;50(3):474-85. doi: 10.1002/prot.10315.
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RecQ family helicases: roles as tumor suppressor proteins.RecQ 家族解旋酶:作为肿瘤抑制蛋白的作用。
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2型腺相关病毒Rep40-ADP复合物的结构:对超家族3解旋酶核苷酸识别和催化作用的深入了解。

Structure of adeno-associated virus type 2 Rep40-ADP complex: insight into nucleotide recognition and catalysis by superfamily 3 helicases.

作者信息

James J Anson, Aggarwal Aneel K, Linden R Michael, Escalante Carlos R

机构信息

Structural Biology Program, Department of Physiology and Biophysics, and Departments of Gene and Cell Medicine and Microbiology, Mount Sinai School of Medicine, 1 Gustave L. Levy Place, New York, NY 10029, USA.

出版信息

Proc Natl Acad Sci U S A. 2004 Aug 24;101(34):12455-60. doi: 10.1073/pnas.0403454101. Epub 2004 Aug 13.

DOI:10.1073/pnas.0403454101
PMID:15310852
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC515083/
Abstract

We have determined the structure of adeno-associated virus type 2 (AAV2) Rep40 to 2.1-A resolution with ADP bound at the active site. The complex crystallizes as a monomer with one ADP molecule positioned in an unexpectedly open binding site. The nucleotide-binding pocket consists of the P-loop residues interacting with the phosphates and a loop (nucleoside-binding loop) that emanates from the last strand of the central beta-sheet and interacts with the sugar and base. As a result of the open nature of the binding site, one face of the adenine ring is completely exposed to the solvent, and consequently the number of protein-nucleotide contacts is scarce as compared with other P-loop nucleotide phosphohydrolases. The conformation of the ADP molecule in its binding site bears a resemblance to those found in only three other families of P-loop ATPases: the ATP-binding cassette transporter family, the bacterial RecA proteins, and the type II topoisomerase family. In all these cases, oligomerization is required to attain a competent nucleotide-binding pocket. We propose that this characteristic is native to superfamily 3 helicases and allows for an additional mechanism of regulation by these multifunctional proteins. Furthermore, it explains the strong tendency by members of this family such as simian virus 40 TAg to oligomerize after binding ATP.

摘要

我们已经确定了2型腺相关病毒(AAV2)Rep40与结合在活性位点的ADP的结构,分辨率达到2.1埃。该复合物以单体形式结晶,一个ADP分子位于一个出人意料的开放结合位点。核苷酸结合口袋由与磷酸相互作用的P环残基和一个从中央β折叠的最后一条链发出并与糖和碱基相互作用的环(核苷结合环)组成。由于结合位点的开放性质,腺嘌呤环的一个面完全暴露于溶剂中,因此与其他P环核苷酸磷酸水解酶相比,蛋白质-核苷酸的接触数量很少。ADP分子在其结合位点的构象与仅在其他三个P环ATP酶家族中发现的构象相似:ATP结合盒转运蛋白家族、细菌RecA蛋白和II型拓扑异构酶家族。在所有这些情况下,需要寡聚化才能形成合适的核苷酸结合口袋。我们提出,这种特性是超家族3解旋酶所特有的,并且允许这些多功能蛋白有额外的调节机制。此外,这解释了该家族成员如猿猴病毒40大T抗原在结合ATP后强烈的寡聚化倾向。