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首页> 外文期刊>PLoS Genetics >Hypermutability of Damaged Single-Strand DNA Formed at Double-Strand Breaks and Uncapped Telomeres in Yeast Saccharomyces cerevisiae
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Hypermutability of Damaged Single-Strand DNA Formed at Double-Strand Breaks and Uncapped Telomeres in Yeast Saccharomyces cerevisiae

机译:酵母酵母中双链断裂和不封端的端粒形成的受损单链DNA的超突变性。

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摘要

The major DNA repair pathways operate on damage in double-strand DNA because they use the intact strand as a template after damage removal. Therefore, lesions in transient single-strand stretches of chromosomal DNA are expected to be especially threatening to genome stability. To test this hypothesis, we designed systems in budding yeast that could generate many kilobases of persistent single-strand DNA next to double-strand breaks or uncapped telomeres. The systems allowed controlled restoration to the double-strand state after applying DNA damage. We found that lesions induced by UV-light and methyl methanesulfonate can be tolerated in long single-strand regions and are hypermutagenic. The hypermutability required PCNA monoubiquitination and was largely attributable to translesion synthesis by the error-prone DNA polymerase ζ. In support of multiple lesions in single-strand DNA being a source of hypermutability, analysis of the UV-induced mutants revealed strong strand-specific bias and unexpectedly high frequency of alleles with widely separated multiple mutations scattered over several kilobases. Hypermutability and multiple mutations associated with lesions in transient stretches of long single-strand DNA may be a source of carcinogenesis and provide selective advantage in adaptive evolution.
机译:主要的DNA修复途径对双链DNA的损伤起作用,因为它们在损伤去除后将完整的链用作模板。因此,预期染色体DNA的瞬时单链延伸中的损伤特别威胁基因组稳定性。为了验证该假设,我们在发芽酵母中设计了系统,该系统可以在双链断裂或无端粒端粒旁边生成许多千碱基的持久性单链DNA。该系统允许在施加DNA损伤后受控恢复至双链状态。我们发现由紫外线和甲磺酸甲酯诱导的病变在长的单链区域中是可以耐受的,并且是高致突变性的。超突变性需要PCNA单泛素化,并且很大程度上归因于易错DNA聚合酶ζ的跨病变合成。为了支持单链DNA中的多个损伤,该突变是超变异性的来源,对UV诱导的突变体的分析显示,强烈的链特异性偏倚和意想不到的高频等位基因具有广泛分布的多个突变,分布在几千个碱基上。超长变异性和与长单链DNA的瞬时延伸中的病变相关的多个突变可能是致癌的来源,并在适应性进化中提供了选择性优势。

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