Melanoma-derived DNA polymerase theta variants exhibit altered DNA polymerase activity

Corey Thomas, Lisbeth Avalos-Irving, Jorge Victorino, Sydney Green, Morgan Andrews, Naisha Rodrigues, Sarah Ebirim, Ayden Mudd, Jamie B Towle-Weicksel
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Abstract

DNA Polymerase θ (Pol θ or POLQ) is primarily involved in repairing double-stranded breaks in DNA through the alternative pathway known as microhomology-mediated end joining (MMEJ) or theta-mediated end joining (TMEJ). Unlike other DNA repair polymerases, Pol θ is thought to be highly error prone, yet critical for cell survival. We have identified several mutations in the POLQ gene from human melanoma tumors. Through biochemical analysis, we have demonstrated that all three cancer-associated variants experienced altered DNA polymerase activity including a propensity for incorrect nucleotide selection and reduced polymerization rates compared to WT Pol θ. Moreover, the variants are 30 fold less efficient at incorporating a nucleotide during repair and up to 70 fold less accurate at selecting the correct nucleotide opposite a templating base. Taken together, this suggests that aberrant Pol θ has reduced DNA repair capabilities and may also contribute to increased mutagenesis. While this may be beneficial to normal cell survival, the variants were identified in established tumors suggesting that cancer cells may use this promiscuous polymerase to its advantage to promote metastasis and drug resistance.
黑色素瘤衍生的DNA聚合酶theta变异表现出改变的DNA聚合酶活性
DNA聚合酶θ (Pol θ或POLQ)主要通过微同源介导的末端连接(MMEJ)或theta介导的末端连接(TMEJ)途径参与DNA双链断裂的修复。与其他DNA修复聚合酶不同,Pol θ被认为是高度容易出错的,但对细胞存活至关重要。我们已经从人类黑色素瘤肿瘤中发现了POLQ基因的几个突变。通过生化分析,我们已经证明,与WT Pol θ相比,所有三种癌症相关变异都经历了DNA聚合酶活性的改变,包括不正确核苷酸选择的倾向和聚合速率的降低。此外,这些变体在修复过程中结合核苷酸的效率降低了30倍,在选择与模板碱基相反的正确核苷酸时的准确性降低了70倍。综上所述,这表明异常的Pol θ降低了DNA修复能力,也可能导致突变增加。虽然这可能有利于正常细胞的存活,但在已建立的肿瘤中发现了这些变异,这表明癌细胞可能利用这种混杂聚合酶来促进转移和耐药性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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