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Isolation of homozygous mutant mouse embryonic stem cells using a dual selection system

机译:使用双重选择系统分离纯合突变型小鼠胚胎干细胞

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摘要

Obtaining random homozygous mutants in mammalian cells for forward genetic studies has always been problematic due to the diploid genome. With one mutation per cell, only one allele of an autosomal gene can be disrupted, and the resulting heterozygous mutant is unlikely to display a phenotype. In cells with a genetic background deficient for the Bloom's syndrome helicase, such heterozygous mutants segregate homozygous daughter cells at a low frequency due to an elevated rate of crossover following mitotic recombination between homologous chromosomes. We constructed DNA vectors that are selectable based on their copy number and used these to isolate these rare homozygous mutant cells independent of their phenotype. We use the piggyBac transposon to limit the initial mutagenesis to one copy per cell, and select for cells that have increased the transposon copy number to two or more. This yields homozygous mutants with two allelic mutations, but also cells that have duplicated the mutant chromosome and become aneuploid during culture. On average, 26% of the copy number gain events occur by the mitotic recombination pathway. We obtained homozygous cells from 40% of the heterozygous mutants tested. This method can provide homozygous mammalian loss-of-function mutants for forward genetic applications.
机译:由于二倍体基因组,在哺乳动物细胞中获得随机纯合突变体进行正向遗传研究一直存在问题。每个细胞只有一个突变,常染色体基因中只有一个等位基因可以被破坏,并且产生的杂合突变体不太可能表现出表型。在遗传背景缺乏布卢姆综合症解旋酶的细胞中,由于同源染色体之间的有丝分裂重组后交叉率升高,这种杂合突变体以较低的频率分离纯合子细胞。我们构建了可根据其拷贝数进行选择的DNA载体,并使用这些载体来分离这些稀有的纯合突变细胞,而与它们的表型无关。我们使用piggyBac转座子将初始诱变限制为每个细胞一个拷贝,并选择将转座子拷贝数增加到两个或更多的细胞。这产生具有两个等位基因突变的纯合突变体,但是也产生了复制突变体染色体并在培养期间变成非整倍体的细胞。平均而言,通过有丝分裂重组途径发生拷贝数增加事件的26%。我们从40%的杂合突变体中获得了纯合细胞。该方法可以提供纯合的哺乳动物功能丧失的突变体,用于正向遗传应用。

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