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人类体细胞和胚胎干细胞群体中的低度染色体嵌合体。

Low-grade chromosomal mosaicism in human somatic and embryonic stem cell populations.

机构信息

Research Group Reproduction and Genetics, Faculty of Medicine and Pharmacy, Vrije Universiteit Brussel (VUB), Laarbeeklaan 101, Brussels 1090, Belgium.

Centre for Medical Genetics, Universitair Ziekenhuis Brussel, Laarbeeklaan 101, 1090, Brussels 1090, Belgium.

出版信息

Nat Commun. 2014 Jun 27;5:4227. doi: 10.1038/ncomms5227.

Abstract

Current knowledge on chromosomal mosaicism in human cell cultures is mostly based on cytogenetic banding methods. The recent development of high-resolution full-genome analysis methods applicable to single cells is providing new insights into genetic and cellular diversity. Here we study the genetic content of 92 individual human cells, including fibroblasts, amniocytes and embryonic stem cells (hESCs), using single-cell array-based comparative genomic hybridization (aCGH). We find that human somatic and embryonic stem cell cultures show significant fractions of cells carrying unique megabase-scale chromosomal abnormalities, forming genetic mosaics that could not have been detected by conventional cytogenetic methods. These findings are confirmed by studying seven clonal hESC sub-lines by aCGH. Furthermore, fluorescent in situ hybridisation reveals an increased instability of the subtelomeric regions in hESC as compared to somatic cells. This genetic heterogeneity may have an impact on experimental results and, in the case of hESC, on their potential clinical use.

摘要

目前关于人类细胞培养中染色体嵌合体的知识主要基于细胞遗传学带型方法。最近开发的适用于单细胞的高分辨率全基因组分析方法为遗传和细胞多样性提供了新的见解。在这里,我们使用单细胞阵列比较基因组杂交(aCGH)研究了 92 个人类细胞,包括成纤维细胞、羊水细胞和胚胎干细胞(hESC)。我们发现,人类体细胞和胚胎干细胞培养物显示出携带独特的兆碱基级染色体异常的细胞的显著分数,形成了不能通过传统细胞遗传学方法检测到的遗传嵌合体。这些发现通过对七个克隆 hESC 亚系进行 aCGH 研究得到了证实。此外,荧光原位杂交显示 hESC 中端粒区比体细胞更不稳定。这种遗传异质性可能会对实验结果产生影响,在 hESC 的情况下,还可能会对其潜在的临床应用产生影响。

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