Somatic copy number mosaicism in human skin revealed by induced pluripotent stem cells

Abyzov, Alexej; Mariani, Jessica; Palejev, Dean; Zhang, Ying; Haney, Michael S.; Tomasini, Livia; Ferrandino, Anthony F.; Belmaker, Lior A. Rosenberg; Székely, Anna; Wilson, Michael; Kocabas, Arif; Calixto, Nathaniel E.; Grigorenko, Elena L.; Hüttner, Anita; Chawarska, Katarzyna; Weissman, Sherman M.; Urban, Alexander; Gerstein, Mark; Vaccarino, Flora M.

doi:10.1038/nature11629

Cited by 347 publications

(290 citation statements)

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“…The size, nature and frequencies of these segmental CNVs are comparable to the abnormalities recently reported in fibroblasts 6 , differentiated hiPSC and neurons studied using aCGH and single-cell sequencing 19 . Remarkably, we only found full chromosome aneuploidy in two hESCs and none in the somatic cells: one hESC contained a trisomy 20 and one was triploid.…”

Section: Detection Of Genetic Imbalances In Single Cells By Acghsupporting

confidence: 59%

“…As these CNVs are present at very low frequencies in the culture, they also could not be detected using the straight-forward analysis of pooled DNA, as used by most studies for high-resolution screening of cell lines. To get around this, Abyzov et al 6 derived hiPSC lines from skin biopsies to clonally amplify the genetic content of single fibroblasts and described low-frequency kilo-base scale CNVs unique to each subclone. This is indicative for low-grade mosaicism in the original fibroblasts; however, the CNVs described by Abyzov et al 6 are considerably smaller than the CNVs described in this study.…”

Section: Discussionmentioning

confidence: 99%

“…To get around this, Abyzov et al 6 derived hiPSC lines from skin biopsies to clonally amplify the genetic content of single fibroblasts and described low-frequency kilo-base scale CNVs unique to each subclone. This is indicative for low-grade mosaicism in the original fibroblasts; however, the CNVs described by Abyzov et al 6 are considerably smaller than the CNVs described in this study. A very recent publication reports genetic mosaicism of megabase-scale CNVs in differentiated hiPSC, cultured fibroblasts and neurons using various high-resolution single-cell genomics 19 .…”

Section: Discussionmentioning

confidence: 99%

“…These studies have shown that the grade of mosaicism varies from tissue to tissue and the percentage of aneuploid cells increases with age, but provide limited insight on the occurrence of small genetic imbalances [2][3][4][5] . More recently, the group of Abyzov et al 6 made use of the clonal nature of humaninduced pluripotent stem cells (hiPSCs) to show that human skin fibroblasts are highly mosaic, with up to 30% of cells carrying copy number variants (CNVs). In the field of human pluripotent stem cell research, a large number of studies have shown that human embryonic stem cell (hESC) cultures are frequently taken over by chromosomally abnormal cells 7,8 , most probably because of a selective advantage caused by the chromosomal aberration 9,10 .…”

mentioning

confidence: 99%

“…In recent years, many groups have performed high-resolution screening of somatic cell populations 1,6,11,12 as well as hiPSC and hESC 7,8 and have reported de novo CNVs ranging from 10 kb to several Mb. It is important to bear in mind that these studies are based on the analysis of DNA from extractions from large numbers of cells, which only allows detection of CNVs if they are present in at least 5-10% of the cells 11,12 .…”

mentioning

confidence: 99%

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

et al. 2014

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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.

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Section: Detection Of Genetic Imbalances In Single Cells By Acghsupporting

confidence: 59%

Section: Discussionmentioning

confidence: 99%