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腺相关病毒rep的核酸酶结构域利用两个不同的DNA识别界面来协调复制起始。

The nuclease domain of adeno-associated virus rep coordinates replication initiation using two distinct DNA recognition interfaces.

作者信息

Hickman Alison Burgess, Ronning Donald R, Perez Zhanita N, Kotin Robert M, Dyda Fred

机构信息

Laboratory of Molecular Biology, National Institute of Diabetes and Digestive and Kidney Diseases, National Institutes of Health, Bethesda, MD 20892 USA.

出版信息

Mol Cell. 2004 Feb 13;13(3):403-14. doi: 10.1016/s1097-2765(04)00023-1.

Abstract

Integration into a particular location in human chromosomes is a unique property of the adeno-associated virus (AAV). This reaction requires the viral Rep protein and AAV origin sequences. To understand how Rep recognizes DNA, we have determined the structures of the Rep endonuclease domain separately complexed with two DNA substrates: the Rep binding site within the viral inverted terminal repeat and one of the terminal hairpin arms. At the Rep binding site, five Rep monomers bind five tetranucleotide direct repeats; each repeat is recognized by two Rep monomers from opposing faces of the DNA. Stem-loop binding involves a protein interface on the opposite side of the molecule from the active site where ssDNA is cleaved. Rep therefore has three distinct binding sites within its endonuclease domain for its different DNA substrates. Use of these different interfaces generates the structural asymmetry necessary to regulate later events in viral replication and integration.

摘要

整合到人类染色体的特定位置是腺相关病毒(AAV)的独特特性。该反应需要病毒Rep蛋白和AAV起源序列。为了了解Rep如何识别DNA,我们分别测定了Rep核酸内切酶结构域与两种DNA底物复合的结构:病毒反向末端重复序列内的Rep结合位点和末端发夹臂之一。在Rep结合位点,五个Rep单体结合五个四核苷酸直接重复序列;每个重复序列由来自DNA相对面的两个Rep单体识别。茎环结合涉及分子中与切割单链DNA的活性位点相对的一侧的蛋白质界面。因此,Rep在其核酸内切酶结构域内具有三个不同的结合位点用于其不同的DNA底物。使用这些不同的界面产生了调节病毒复制和整合后期事件所需的结构不对称性。

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