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DNA Polymerase θ: A Unique Multifunctional End-Joining Machine

机译:DNA Polymeraseθ:独特的多功能末端连接机

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摘要

The gene encoding DNA polymerase θ (Polθ) was discovered over ten years ago as having a role in suppressing genome instability in mammalian cells. Studies have now clearly documented an essential function for this unique A-family polymerase in the double-strand break (DSB) repair pathway alternative end-joining (alt-EJ), also known as microhomology-mediated end-joining (MMEJ), in metazoans. Biochemical and cellular studies show that Polθ exhibits a unique ability to perform alt-EJ and during this process the polymerase generates insertion mutations due to its robust terminal transferase activity which involves template-dependent and independent modes of DNA synthesis. Intriguingly, the POLQ gene also encodes for a conserved superfamily 2 Hel308-type ATP-dependent helicase domain which likely assists in alt-EJ and was reported to suppress homologous recombination (HR) via its anti-recombinase activity. Here, we review our current knowledge of Polθ-mediated end-joining, the specific activities of the polymerase and helicase domains, and put into perspective how this multifunctional enzyme promotes alt-EJ repair of DSBs formed during S and G2 cell cycle phases.
机译:十年前发现了编码DNA聚合酶θ(Polθ)的基因,它具有抑制哺乳动物细胞中基因组不稳定的作用。现在的研究清楚地证明了这种独特的A族聚合酶在双链断裂(DSB)修复途径的替代末端连接(alt-EJ)(也称为微同源介导的末端连接(MMEJ))中的基本功能。后生动物。生化和细胞研究表明,Polθ表现出独特的执行alt-EJ的能力,在此过程中,聚合酶由于其强大的末端转移酶活性(涉及模板依赖和独立的DNA合成模式)而产生插入突变。有趣的是,POLQ基因还编码一个保守的超家族2 Hel308型ATP依赖性解旋酶结构域,该结构域可能有助于alt-EJ,并据报道可通过其抗重组酶活性抑制同源重组(HR)。在这里,我们回顾了我们目前对Polθ介导的末端连接,聚合酶和解旋酶结构域的比活性的了解,并透视了这种多功能酶如何促进在S和G2细胞周期阶段形成的DSB的alt-EJ修复。

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