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首页> 外文期刊>Progress in nucleic acid research and molecular biology >Fidelity mechanisms of DNA polymerase beta.
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Fidelity mechanisms of DNA polymerase beta.

机译:DNA聚合酶β的保真机制。

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摘要

DNA polymerase 3 (Pol beta) is one of the best characterized eukaryotic DNA polymerases. Pol beta is a member of the X family of DNA polymerases. The Pol beta protein has two catalytic activities: DNA polymerase activity and dRP lyase activity. Pol beta has no known proofreading activity, so its accuracy in vitro results exclusively from the nucleotide selectivity of this enzyme. Presteady-state kinetic analysis has shown that Pol beta functions in nucleotide selectivity predominantly during phosphodiester bond formation, although this enzyme also possesses some ability to discriminate the correct from the incorrect deoxynucleoside triphosphate (dNTP) substrate during ground state binding. Recent results strongly suggest that Pol beta does not employ an induced fit mechanism of nucleotide discrimination. The fidelity of Pol beta appears to be determined through steric exclusion against the incorrect substrate and by the precise positioning of the catalytic residues, DNA, and substrate within the activesite of the enzyme. Imprecise positioning of active site residues or DNA can result in the incorporation of the incorrect substrate into DNA. Amino acid residues both distant and near to the active site of Pol beta influence its geometry, suggesting that the movements and positioning of subdomains of Pol beta have a significant impact upon its fidelity.
机译:DNA聚合酶3(Pol beta)是最具特征的真核DNA聚合酶之一。 Pol beta是DNA聚合酶X家族的成员。 Polβ蛋白具有两种催化活性:DNA聚合酶活性和dRP裂解酶活性。 Pol beta没有已知的校对活性,因此其体外准确性仅由该酶的核苷酸选择性决定。前稳态动力学分析表明,Polβ主要在磷酸二酯键形成过程中发挥核苷酸选择性的作用,尽管该酶还具有在基态结合过程中将正确的与错误的脱氧核苷三磷酸(dNTP)底物区分开的能力。最近的结果有力地表明,Pol beta不采用核苷酸区分的诱导拟合机制。 Polβ的保真度似乎是通过针对不正确的底物的空间排阻以及催化残基,DNA和底物在酶活性位点内的精确定位来确定的。活性位点残基或DNA的不正确定位会导致将错误的底物掺入DNA中。 Polβ活性位点的远处和附近的氨基酸残基都会影响其几何形状,这表明Polβ的亚域的移动和位置对其保真度有重要影响。

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