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Variation of mutational burden in healthy human tissues suggests non-random strand segregation and allows measuring somatic mutation rates

机译:健康人体组织中突变负荷的变化表明存在非随机链分离,并允许测量体细胞突变率

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Author summary Cairn proposed in 1975 that upon proliferation, cells might not segregate DNA strands randomly into daughter cells, but preferentially keep the ancestral (blue print) template strand in stem cells. This mechanism would allow to drastically reduce the rate of mutation accumulation in human tissues. Testing the hypothesis in human stem cells within their natural tissue environment remains challenging. Here we show that the patterns of mutation accumulation in human tissues with age support highly effective non-random DNA strand segregation after adolescence. In contrast, during early development in infants, DNA strand segregation is less effective, likely because stem cell populations are continuing to grow.
机译:作者总结凯恩(Cairn)在1975年提出,细胞增殖后可能不会将DNA链随机地分离成子细胞,而是优先将祖先(蓝图)模板链保留在干细胞中。这种机制将允许大大降低人体组织中突变积累的速率。在自然组织环境中测试人类干细胞的假设仍然具有挑战性。在这里,我们显示,随着年龄的增长,人体组织中的突变积累模式支持青春期后的高效非随机DNA链分离。相反,在婴儿的早期发育过程中,DNA链的分离效果较差,这可能是因为干细胞群体正在持续增长。

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