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首页> 外文期刊>Nucleic Acids Research >Direct, genome-wide assessment of DNA mutations in single cells
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Direct, genome-wide assessment of DNA mutations in single cells

机译:直接,全基因组评估单个细胞中的DNA突变

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摘要

DNA mutations are the inevitable consequences of errors that arise during replication and repair of DNA damage. Because of their random and infrequent occurrence, quantification and characterization of DNA mutations in the genome of somatic cells has been difficult. Random, low-abundance mutations are currently inaccessible by standard high-throughput sequencing approaches because they cannot be distinguished from sequencing errors. One way to circumvent this problem and simultaneously account for the mutational heterogeneity within tissues is whole genome sequencing of a representative number of single cells. Here, we show elevated mutation levels in single cells from Drosophila melanogaster S2 and mouse embryonic fibroblast populations after treatment with the powerful mutagen N-ethyl-N-nitrosourea. This method can be applied as a direct measure of exposure to mutagenic agents and for assessing genotypic heterogeneity within tissues or cell populations.
机译:DNA突变是DNA损伤的复制和修复过程中出现错误的必然结果。由于它们的随机发生和不频繁发生,很难对体细胞基因组中的DNA突变进行定量和表征。目前,标准的高通量测序方法无法获得随机,低丰度的突变,因为它们无法与测序错误区分开。规避此问题并同时说明组织内突变异质性的一种方法是对代表性数量的单细胞进行全基因组测序。在这里,我们显示了强大的诱变剂N-乙基-N-亚硝基脲处理后,果蝇S2和小鼠胚胎成纤维细胞群体中单细胞的突变水平升高。该方法可以用作直接接触诱变剂的方法,也可以用于评估组织或细胞群体内的基因型异质性。

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