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人类 Pol ι 多态变体的 DNA 聚合酶和 dRP 裂解酶活性。

DNA Polymerase and dRP-lyase activities of polymorphic variants of human Pol ι.

机构信息

Institute of Molecular Genetics, National Research Center «Kurchatov Institute», Kurchatov sq. 2, 123182 Moscow, Russia.

Institute of Genetics and Cytology of the National Academy of Sciences of Belarus, 220072 Minsk, Republic of Belarus.

出版信息

Biochem J. 2021 Apr 16;478(7):1399-1412. doi: 10.1042/BCJ20200491.

Abstract

Y-family DNA polymerase iota (Pol ι) is involved in DNA damage response and tolerance. Mutations and altered expression level of POLI gene are linked to a higher incidence of cancer. We biochemically characterized five active site polymorphic variants of human Pol ι: R71G (rs3218778), P118L (rs554252419), I236M (rs3218784), E251K (rs3218783) and P365R (rs200852409). We analyzed fidelity of nucleotide incorporation on undamaged DNA, efficiency and accuracy of DNA damage bypass, as well as 5'-deoxyribophosphate lyase (dRP-lyase) activity. The I236M and P118L variants were indistinguishable from the wild-type Pol ι in activity. The E251K and P365R substitutions altered the spectrum of nucleotide incorporation opposite several undamaged DNA bases. The P365R variant also reduced the dRP-lyase activity and possessed the decreased TLS activity opposite 8-oxo-G. The R71G mutation dramatically affected the catalytic activities of Pol ι. The reduced DNA polymerase activity of the R71G variant correlated with an enhanced fidelity of nucleotide incorporation on undamaged DNA, altered lesion-bypass activity and reduced dRP-lyase activity. Therefore, this amino acid substitution likely alters Pol ι functions in vivo.

摘要

Y 家族 DNA 聚合酶 ι(Pol ι)参与 DNA 损伤反应和耐受。POLI 基因突变和表达水平改变与癌症发病率升高有关。我们对人 Pol ι 的五个活性位点多态性变体进行了生化表征:R71G(rs3218778)、P118L(rs554252419)、I236M(rs3218784)、E251K(rs3218783)和 P365R(rs200852409)。我们分析了在未受损 DNA 上核苷酸掺入的保真度、DNA 损伤绕过的效率和准确性,以及 5'-脱氧核糖磷酸解酶(dRP- 裂合酶)活性。I236M 和 P118L 变体在活性方面与野生型 Pol ι 无法区分。E251K 和 P365R 取代改变了几种未受损 DNA 碱基的核苷酸掺入谱。P365R 变体还降低了 dRP-裂合酶活性,并降低了对 8-氧代-G 的 TLS 活性。R71G 突变极大地影响了 Pol ι 的催化活性。R71G 变体的 DNA 聚合酶活性降低与未受损 DNA 上核苷酸掺入保真度提高、损伤绕过活性改变和 dRP-裂合酶活性降低相关。因此,这种氨基酸取代可能会改变 Pol ι 在体内的功能。

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