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非典型原核 X 家族 DNA 聚合酶缺乏聚合酶活性,而充当核酸外切酶。

Noncanonical prokaryotic X family DNA polymerases lack polymerase activity and act as exonucleases.

机构信息

Institute of Molecular Genetics, National Research Centre "Kurchatov Institute", Moscow 123182, Russia.

出版信息

Nucleic Acids Res. 2022 Jun 24;50(11):6398-6413. doi: 10.1093/nar/gkac461.

Abstract

The X family polymerases (PolXs) are specialized DNA polymerases that are found in all domains of life. While the main representatives of eukaryotic PolXs, which have dedicated functions in DNA repair, were studied in much detail, the functions and diversity of prokaryotic PolXs have remained largely unexplored. Here, by combining a comprehensive bioinformatic analysis of prokaryotic PolXs and biochemical experiments involving selected recombinant enzymes, we reveal a previously unrecognized group of PolXs that seem to be lacking DNA polymerase activity. The noncanonical PolXs contain substitutions of the key catalytic residues and deletions in their polymerase and dNTP binding sites in the palm and fingers domains, but contain functional nuclease domains, similar to canonical PolXs. We demonstrate that representative noncanonical PolXs from the Deinococcus genus are indeed inactive as DNA polymerases but are highly efficient as 3'-5' exonucleases. We show that both canonical and noncanonical PolXs are often encoded together with the components of the non-homologous end joining pathway and may therefore participate in double-strand break repair, suggesting an evolutionary conservation of this PolX function. This is a remarkable example of polymerases that have lost their main polymerase activity, but retain accessory functions in DNA processing and repair.

摘要

X 家族聚合酶(PolXs)是存在于所有生命领域的专门的 DNA 聚合酶。虽然真核 PolXs 的主要代表在 DNA 修复中具有专门的功能,并进行了详细的研究,但原核 PolXs 的功能和多样性在很大程度上仍未得到探索。在这里,我们通过对原核 PolXs 的综合生物信息学分析和涉及选定重组酶的生化实验,揭示了一组以前未被识别的似乎缺乏 DNA 聚合酶活性的 PolXs。这些非典型的 PolXs 包含关键催化残基的取代以及 palm 和 fingers 结构域中聚合酶和 dNTP 结合位点的缺失,但包含类似于典型 PolXs 的功能核酸酶结构域。我们证明,来自 Deinococcus 属的代表性非典型 PolXs 实际上作为 DNA 聚合酶是无活性的,但作为 3'-5' 外切核酸酶却是高效的。我们表明,无论是典型的还是非典型的 PolXs 通常都与非同源末端连接途径的成分一起被编码,因此可能参与双链断裂修复,这表明这种 PolX 功能在进化上是保守的。这是一个显著的例子,说明了聚合酶失去了其主要的聚合酶活性,但在 DNA 加工和修复中保留了辅助功能。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/beb5/9226535/3ce2a4465667/gkac461fig1.jpg

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