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polVR391的特性:一种由IncJ接合转座子R391的rumA'B编码的Y家族聚合酶。

Characterization of polVR391: a Y-family polymerase encoded by rumA'B from the IncJ conjugative transposon, R391.

作者信息

Mead Samantha, Vaisman Alexandra, Valjavec-Gratian Majda, Karata Kiyonobu, Vandewiele Dominique, Woodgate Roger

机构信息

Laboratory of Genomic Integrity, National Institute of Child Health and Human Development, National Institutes of Health, Bethesda, MD 20892-2725, USA.

出版信息

Mol Microbiol. 2007 Feb;63(3):797-810. doi: 10.1111/j.1365-2958.2006.05561.x.

Abstract

Although best characterized for their ability to traverse a variety of DNA lesions, Y-family DNA polymerases can also give rise to elevated spontaneous mutation rates if they are allowed to replicate undamaged DNA. One such enzyme that promotes high levels of spontaneous mutagenesis in Escherichia coli is polV(R391), a polV-like Y-family polymerase encoded by rumA'B from the IncJ conjugative transposon R391. When expressed in a DeltaumuDC lexA(Def) recA730 strain, polV(R391) promotes higher levels of spontaneous mutagenesis than the related MucA'B (polR1) or UmuD'C (polV) polymerases respectively. Analysis of the spectrum of polV(R391)-dependent mutations in rpoB revealed a unique genetic fingerprint that is typified by an increase in C:G-->A:T and A:T-->T:A transversions at certain mutagenic hot spots. Biochemical characterization of polV(R391) highlights the exceptional ability of the enzyme to misincorporate T opposite C and T in sequence contexts corresponding to mutagenic hot spots. Purified polV(R391) can also bypass a T-T pyrimidine dimer efficiently and displays greater accuracy opposite the 3'T of the dimer than opposite an undamaged T. Our study therefore provides evidence for the molecular basis for the enhanced spontaneous mutator activity of RumA'B, as well as explains its ability to promote efficient and accurate bypass of T-T pyrimidine dimers in vivo.

摘要

尽管Y家族DNA聚合酶最显著的特点是能够跨越多种DNA损伤,但如果让它们复制未受损的DNA,也会导致自发突变率升高。在大肠杆菌中促进高水平自发诱变的一种这样的酶是polV(R391),它是一种由IncJ接合转座子R391的rumA'B编码的polV样Y家族聚合酶。当在DeltaumuDC lexA(Def) recA730菌株中表达时,polV(R391)分别比相关的MucA'B (polR1)或UmuD'C (polV)聚合酶促进更高水平的自发诱变。对rpoB中依赖polV(R391)的突变谱分析揭示了一种独特的遗传指纹,其特征是在某些诱变热点处C:G-->A:T和A:T-->T:A颠换增加。polV(R391)的生化特性突出了该酶在对应于诱变热点的序列环境中错误掺入与C和T相对的T的特殊能力。纯化的polV(R391)也能有效地绕过T-T嘧啶二聚体,并且与未受损的T相比,在二聚体的3'T处显示出更高的准确性。因此,我们的研究为RumA'B增强的自发诱变活性的分子基础提供了证据,并解释了其在体内促进T-T嘧啶二聚体有效和准确绕过的能力。

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