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裂殖酵母中Rpa1/Ssb1检查点信号功能的全面突变分析。

Comprehensive mutational analysis of the checkpoint signaling function of Rpa1/Ssb1 in fission yeast.

作者信息

Xu Yong-Jie, Bhadra Sankhadip, Mahdi Alaa Taha A, Dev Kamal, Yurtsever Ilknur, Nakamura Toru M

机构信息

Department of Pharmacology and Toxicology, Boonshoft School of Medicine, Wright State University, Dayton, Ohio, USA.

Department of Biochemistry and Molecular Genetics, University of Illinois at Chicago, Chicago, Illinois, USA.

出版信息

bioRxiv. 2023 Mar 6:2023.03.06.531248. doi: 10.1101/2023.03.06.531248.

Abstract

UNLABELLED

Replication protein A (RPA) is a heterotrimeric complex and the major single-strand DNA (ssDNA) binding protein in eukaryotes. It plays important roles in DNA replication, repair, recombination, telomere maintenance, and checkpoint signaling. Because RPA is essential for cell survival, understanding its checkpoint signaling function in cells has been challenging. Several RPA mutants have been reported previously in fission yeast. None of them, however, has a defined checkpoint defect. A separation-of-function mutant of RPA, if identified, would provide significant insights into the checkpoint initiation mechanisms. We have explored this possibility and carried out an extensive genetic screening for Rpa1/Ssb1, the large subunit of RPA in fission yeast, looking for mutants with defects in checkpoint signaling. This screen has identified twenty-five primary mutants that are sensitive to genotoxins. Among these mutants, two have been confirmed partially defective in checkpoint signaling primarily at the replication fork, not the DNA damage site. The remaining mutants are likely defective in other functions such as DNA repair or telomere maintenance. Our screened mutants, therefore, provide a valuable tool for future dissection of the multiple functions of RPA in fission yeast.

AUTHOR SUMMARY

Originally discovered as a protein required for replication of simian virus SV40 DNA, replication protein A is now known to function in DNA replication, repair, recombination, telomere maintenance, and checkpoint signaling in all eukaryotes. The protein is a complex of three subunits and the two larger ones are essential for cell growth. This essential function however complicates the studies in living cells, and for this reason, its checkpoint function remains to be fully understood. We have carried out an genetic screening of the largest subunit of this protein in fission yeast, aiming to find a non-lethal mutant that lacks the checkpoint function. This extensive screen has uncovered two mutants with a partial defect in checkpoint signaling when DNA replication is arrested. Surprisingly, although the two mutants also have a defect in DNA repair, their checkpoint signaling remains largely functional in the presence of DNA damage. We have also uncovered twenty-three mutants with defects in DNA repair or telomere maintenance, but not checkpoint signaling. Therefore, the non-lethal mutants uncovered by this study provide a valuable tool for dissecting the multiple functions of this biologically important protein in fission yeast.

摘要

未标记

复制蛋白A(RPA)是一种异源三聚体复合物,是真核生物中主要的单链DNA(ssDNA)结合蛋白。它在DNA复制、修复、重组、端粒维持和检查点信号传导中发挥重要作用。由于RPA对细胞存活至关重要,因此了解其在细胞中的检查点信号传导功能一直具有挑战性。此前在裂殖酵母中已报道了几种RPA突变体。然而,它们中没有一个具有明确的检查点缺陷。如果能鉴定出RPA的功能分离突变体,将为检查点启动机制提供重要见解。我们探索了这种可能性,并对裂殖酵母中RPA的大亚基Rpa1/Ssb1进行了广泛的遗传筛选,寻找检查点信号传导有缺陷的突变体。该筛选鉴定出了25个对基因毒素敏感的初级突变体。在这些突变体中,有两个已被证实主要在复制叉处而非DNA损伤位点的检查点信号传导存在部分缺陷。其余突变体可能在DNA修复或端粒维持等其他功能方面存在缺陷。因此,我们筛选出的突变体为未来剖析RPA在裂殖酵母中的多种功能提供了有价值的工具。

作者总结

复制蛋白A最初被发现是猿猴病毒SV40 DNA复制所需的一种蛋白质,现在已知它在所有真核生物的DNA复制、修复、重组、端粒维持和检查点信号传导中发挥作用。该蛋白是由三个亚基组成的复合物,其中两个较大的亚基对细胞生长至关重要。然而,这种基本功能使在活细胞中的研究变得复杂,因此,其检查点功能仍有待充分了解。我们对裂殖酵母中这种蛋白的大亚基进行了遗传筛选,旨在找到一个缺乏检查点功能的非致死突变体。这项广泛的筛选发现了两个在DNA复制停滞时检查点信号传导存在部分缺陷的突变体。令人惊讶的是,尽管这两个突变体在DNA修复方面也存在缺陷,但在存在DNA损伤的情况下,它们的检查点信号传导仍基本保持功能。我们还发现了23个在DNA修复或端粒维持方面存在缺陷但检查点信号传导无缺陷的突变体。因此,本研究发现的非致死突变体为剖析这种在生物学上重要的蛋白在裂殖酵母中的多种功能提供了有价值的工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/cfec/10028789/56a9f4d6f8f2/nihpp-2023.03.06.531248v1-f0001.jpg

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