首页> 外文期刊>Proceedings of the National Academy of Sciences of the United States of America >Different mutation signatures in DNA polymerase eta(-) and MSH6-deficient mice suggest separate roles in antibody diversification
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Different mutation signatures in DNA polymerase eta(-) and MSH6-deficient mice suggest separate roles in antibody diversification

机译:DNA聚合酶eta(-)和MSH6缺陷小鼠中的不同突变特征表明抗体多样化中的不同作用

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摘要

Hypermutation in immunoglobulin genes produces a high frequency of substitutions of all four bases, which are likely generated by low-fidelity DNA polymerases. Indeed, humans deficient for DNA polymerase (pol) eta have decreased substitutions of A-T base pairs in variable and switch regions. To study the role of pol eta in a genetically tractable system, we created mice lacking pol eta. B cells from Polh(-/-) mice produced normal amounts of IgG, indicating that pol eta does not affect class switch recombination. Similar to their human counterparts, variable and switch regions from Polh(-/-) mice had fewer substitutions of A-T base pairs and correspondingly more mutations of C-G base pairs, which firmly establishes a central role for pol eta in hypermutation. Notably, the location and types of substitutions differ markedly from those in Msh6(-/-) clones, which also have fewer A-T mutations. The data suggest that pol eta preferentially synthesizes a repair patch on the nontranscribed strand, whereas MSH6 functions to generate the patch.
机译:免疫球蛋白基因的超突变产生所有四个碱基的高频率取代,这很可能是由低保真DNA聚合酶产生的。确实,缺乏DNA聚合酶(pol)eta的人类在可变区和转换区中A-T碱基对的取代减少。为了研究pol eta在遗传易处理系统中的作用,我们创建了缺乏pol eta的小鼠。来自Polh(-/-)小鼠的B细胞产生正常量的IgG,表明pol eta不会影响分类开关重组。与人类人类相似,来自Polh(-/-)小鼠的可变区和开关区具有较少的A-T碱基对取代,并具有更多的C-G碱基对突变,从而牢固地确立了pol eta在超突变中的核心作用。值得注意的是,取代的位置和类型与Msh6(-/-)克隆中的A-T突变也少得多。数据表明,pol eta优先在非转录链上合成修复补丁,而MSH6则用于生成补丁。

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