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8-氧代鸟嘌呤与甲酰胺嘧啶-DNA糖基化酶结合模式的计算分析。

Computational analysis of the mode of binding of 8-oxoguanine to formamidopyrimidine-DNA glycosylase.

作者信息

Song Kun, Hornak Viktor, de Los Santos Carlos, Grollman Arthur P, Simmerling Carlos

机构信息

Department of Chemistry, Stony Brook University, Stony Brook, New York 11794-3400, USA.

出版信息

Biochemistry. 2006 Sep 12;45(36):10886-94. doi: 10.1021/bi060380m.

Abstract

8-Oxoguanine (8OG) is the most prevalent form of oxidative DNA damage. In bacteria, 8OG is excised by formamidopyrimidine glycosylase (Fpg) as the initial step in base excision repair. To efficiently excise this lesion, Fpg must discriminate between 8OG and an excess of guanine in duplex DNA. In this study, we explore the structural basis underlying this high degree of selectivity. Two structures have been reported in which Fpg is bound to DNA, differing with respect to the position of the lesion in the active site, one structure showing 8OG bound in the syn conformation and the other in the anti conformation. Remarkably, the results of our all-atom simulations are consistent with both structures. The syn conformation observed in the crystallographic structure of Fpg obtained from Bacillus stearothermophilus is stabilized through interaction with E77, a nonconserved residue. Replacement of E77 with Ser, creating the Fpg sequence found in Escherichia coli and other bacteria, results in preferred binding of 8OG in the anti conformation. Our calculations provide novel insights into the roles of active site residues in binding and recognition of 8OG by Fpg.

摘要

8-氧代鸟嘌呤(8OG)是氧化性DNA损伤最常见的形式。在细菌中,8OG由甲酰胺嘧啶糖基化酶(Fpg)切除,作为碱基切除修复的第一步。为了有效切除这种损伤,Fpg必须在双链DNA中区分8OG和过量的鸟嘌呤。在本研究中,我们探索了这种高度选择性背后的结构基础。已经报道了两种Fpg与DNA结合的结构,它们在活性位点损伤的位置上有所不同,一种结构显示8OG以顺式构象结合,另一种以反式构象结合。值得注意的是,我们的全原子模拟结果与这两种结构都一致。在嗜热脂肪芽孢杆菌获得的Fpg晶体结构中观察到的顺式构象通过与E77(一个非保守残基)的相互作用而稳定。用Ser取代E77,产生在大肠杆菌和其他细菌中发现的Fpg序列,导致8OG优先以反式构象结合。我们的计算为活性位点残基在Fpg结合和识别8OG中的作用提供了新的见解。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/df94/8295719/62a9e5dd4708/nihms93292f1.jpg

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