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Role of human DNA polymerase kappa in extension opposite from a cis-syn thymine dimer.

机译:人类DNA聚合酶kappa在与顺式-胸腺嘧啶二聚体相反的延伸中的作用。

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摘要

Exposure of DNA to UV radiation causes covalent linkages between adjacent pyrimidines. The most common lesion found in DNA from these UV-induced linkages is the cis-syn cyclobutane pyrimidine dimer. Human DNA polymerase kappa (Polkappa), a member of the Y-family of DNA polymerases, is unable to insert nucleotides opposite the 3'T of a cis-syn T-T dimer, but it can efficiently extend from a nucleotide inserted opposite the 3'T of the dimer by another DNA polymerase. We present here the structure of human Polkappa in the act of inserting a nucleotide opposite the 5'T of the cis-syn T-T dimer. The structure reveals a constrained active-site cleft that is unable to accommodate the 3'T of a cis-syn T-T dimer but is remarkably well adapted to accommodate the 5'T via Watson-Crick base pairing, in accord with a proposed role for Polkappa in the extension reaction opposite from cyclobutane pyrimidine dimers in vivo.
机译:DNA暴露于紫外线辐射会导致相邻嘧啶之间的共价键合。这些紫外线诱导的键合在DNA中发现的最常见的病变是顺式-顺式环丁烷嘧啶二聚体。人类DNA聚合酶kappa(Polkappa)是DNA聚合酶Y家族的成员,无法插入与顺式syn TT二聚体3'T相对的核苷酸,但它可以有效地从与3'T相对的核苷酸延伸另一个DNA聚合酶的二聚体的T我们在这里介绍人Polkappa的结构,其行为是插入与顺式Syn T-T二聚体5'T相反的核苷酸。该结构揭示了受约束的活性位点裂隙,无法容纳顺式-顺式TT二聚体的3'T,但非常适合通过Watson-Crick碱基配对容纳5'T,与拟议的作用延伸反应中的Polkappa与体内的环丁烷嘧啶二聚体相反。

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