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哺乳动物DNA聚合酶ζ的聚合酶活性是细胞和胚胎生存能力所特别需要的。

The Polymerase Activity of Mammalian DNA Pol ζ Is Specifically Required for Cell and Embryonic Viability.

作者信息

Lange Sabine S, Tomida Junya, Boulware Karen S, Bhetawal Sarita, Wood Richard D

机构信息

Department of Epigenetics and Molecular Carcinogenesis, The University of Texas MD Anderson Cancer Center, Smithville, Texas, United States of America.

The Graduate School of Biomedical Sciences at Houston, Houston, Texas, United States of America.

出版信息

PLoS Genet. 2016 Jan 4;12(1):e1005759. doi: 10.1371/journal.pgen.1005759. eCollection 2016 Jan.

Abstract

DNA polymerase ζ (pol ζ) is exceptionally important for maintaining genome stability. Inactivation of the Rev3l gene encoding the polymerase catalytic subunit causes a high frequency of chromosomal breaks, followed by lethality in mouse embryos and in primary cells. Yet it is not known whether the DNA polymerase activity of pol ζ is specifically essential, as the large REV3L protein also serves as a multiprotein scaffold for translesion DNA synthesis via multiple conserved structural domains. We report that Rev3l cDNA rescues the genomic instability and DNA damage sensitivity of Rev3l-null immortalized mouse fibroblast cell lines. A cDNA harboring mutations of conserved catalytic aspartate residues in the polymerase domain of REV3L could not rescue these phenotypes. To investigate the role of REV3L DNA polymerase activity in vivo, a Rev3l knock-in mouse was constructed with this polymerase-inactivating alteration. No homozygous mutant mice were produced, with lethality occurring during embryogenesis. Primary fibroblasts from mutant embryos showed growth defects, elevated DNA double-strand breaks and cisplatin sensitivity similar to Rev3l-null fibroblasts. We tested whether the severe Rev3l-/- phenotypes could be rescued by deletion of DNA polymerase η, as has been reported with chicken DT40 cells. However, Rev3l-/- Polh-/- mice were inviable, and derived primary fibroblasts were as sensitive to DNA damage as Rev3l-/- Polh+/+ fibroblasts. Therefore, the functions of REV3L in maintaining cell viability, embryonic viability and genomic stability are directly dependent on its polymerase activity, and cannot be ameliorated by an additional deletion of pol η. These results validate and encourage the approach of targeting the DNA polymerase activity of pol ζ to sensitize tumors to DNA damaging agents.

摘要

DNA聚合酶ζ(pol ζ)对于维持基因组稳定性异常重要。编码聚合酶催化亚基的Rev3l基因失活会导致染色体断裂频率升高,随后小鼠胚胎和原代细胞会死亡。然而,尚不清楚pol ζ的DNA聚合酶活性是否具有特异性的必要性,因为大型REV3L蛋白还通过多个保守结构域作为跨损伤DNA合成的多蛋白支架。我们报告称,Rev3l cDNA可挽救Rev3l基因缺失的永生化小鼠成纤维细胞系的基因组不稳定性和DNA损伤敏感性。携带REV3L聚合酶结构域中保守催化天冬氨酸残基突变的cDNA无法挽救这些表型。为了研究REV3L DNA聚合酶活性在体内的作用,构建了带有这种聚合酶失活改变的Rev3l基因敲入小鼠。没有产生纯合突变小鼠,胚胎发育过程中出现致死现象。突变胚胎的原代成纤维细胞表现出生长缺陷、DNA双链断裂增加和顺铂敏感性升高,类似于Rev3l基因缺失的成纤维细胞。我们测试了是否可以通过缺失DNA聚合酶η来挽救严重的Rev3l-/-表型,正如鸡DT40细胞所报道的那样。然而,Rev3l-/- Polh-/-小鼠无法存活,其衍生的原代成纤维细胞对DNA损伤的敏感性与Rev3l-/- Polh+/+成纤维细胞相同。因此,REV3L在维持细胞活力、胚胎活力和基因组稳定性方面的功能直接依赖于其聚合酶活性,并且不能通过额外缺失pol η来改善。这些结果验证并鼓励了针对pol ζ的DNA聚合酶活性使肿瘤对DNA损伤剂敏感的方法。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/4c63/4699697/f7ba8560c629/pgen.1005759.g001.jpg

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