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深入了解人类末端脱氧核苷酸转移酶的 DNA 合成机制。

Insight into the mechanism of DNA synthesis by human terminal deoxynucleotidyltransferase.

机构信息

Institute of Chemical Biology and Fundamental Medicine, Siberian Branch of Russian Academy of Sciences, Novosibirsk, Russia.

Institute of Chemical Biology and Fundamental Medicine, Siberian Branch of Russian Academy of Sciences, Novosibirsk, Russia

出版信息

Life Sci Alliance. 2022 Aug 1;5(12):e202201428. doi: 10.26508/lsa.202201428.

Abstract

Terminal deoxynucleotidyltransferase (TdT) is a member of the DNA polymerase X family that is responsible for random addition of nucleotides to single-stranded DNA. We present investigation into the role of metal ions and specific interactions of dNTP with active-site amino acid residues in the mechanisms underlying the recognition of nucleoside triphosphates by human TdT under pre-steady-state conditions. In the elongation mode, the ratios of translocation and dissociation rate constants, as well as the catalytic rate constant were dependent on the nature of the nucleobase. Preferences of TdT in dNTP incorporation were researched by molecular dynamics simulations of complexes of TdT with a primer and dNTP or with the elongated primer. Purine nucleotides lost the "summarised" H-bonding network after the attachment of the nucleotide to the primer, whereas pyrimidine nucleotides increased the number and relative lifetime of H-bonds in the post-catalytic complex. The effect of divalent metal ions on the primer elongation revealed that Me<sup>2+</sup> cofactor can significantly change parameters of the primer elongation by strongly affecting the rate of nucleotide attachment and the polymerisation mode.

摘要

末端脱氧核苷酸转移酶(TdT)是 DNA 聚合酶 X 家族的成员,负责将核苷酸随机添加到单链 DNA 上。我们研究了金属离子在人类 TdT 识别核苷三磷酸的机制中的作用,以及 dNTP 与活性位点氨基酸残基的特定相互作用在预稳态条件下的作用。在延伸模式下,易位和解离速率常数的比值以及催化速率常数取决于碱基的性质。通过 TdT 与引物和 dNTP 或与延伸引物的复合物的分子动力学模拟研究了 TdT 在 dNTP 掺入中的偏好性。嘌呤核苷酸在核苷酸与引物结合后失去了“总结”的氢键网络,而嘧啶核苷酸在催化后复合物中增加了氢键的数量和相对寿命。二价金属离子对引物延伸的影响表明,Me<sup>2+</sup>辅助因子可以通过强烈影响核苷酸附着的速率和聚合模式来显著改变引物延伸的参数。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/296d/9348634/2bf2099d4798/LSA-2022-01428_Fig1.jpg

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