| Literature DB >> 33831558 |
Maike Kosanke1, Katarzyna Osetek1, Alexandra Haase1, Lutz Wiehlmann2, Colin Davenport2, Adrian Schwarzer3, Felix Adams3, Marc-Jens Kleppa3, Axel Schambach3, Sylvia Merkert1, Stephanie Wunderlich1, Sandra Menke1, Marie Dorda2, Ulrich Martin4.
Abstract
Cellular therapies based on induced pluripotent stem cells (iPSCs) come out of age and an increasing number of clinical trials applying iPSC-based transplants are ongoing or in preparation. Recent studies, however, demonstrated a high number of small-scale mutations in iPSCs. Although the mutational load in iPSCs seems to be largely derived from their parental cells, it is still unknown whether reprogramming may enrich for individual mutations that could lead to loss of functionality and tumor formation from iPSC derivatives. 30 hiPSC lines were analyzed by whole exome sequencing. High accuracy amplicon sequencing showed that all analyzed small-scale variants pre-existed in their parental cells and that individual mutations present in small subpopulations of parental cells become enriched among hiPSC clones during reprogramming. Among those, putatively actionable driver mutations affect genes related to cell-cycle control, cell death, and pluripotency and may confer a selective advantage during reprogramming. Finally, a short hairpin RNA (shRNA)-based experimental approach was applied to provide additional evidence for the individual impact of such genes on the reprogramming efficiency. In conclusion, we show that enriched mutations in curated onco- and tumor suppressor genes may account for an increased tumor risk and impact the clinical value of patient-derived hiPSCs.Entities:
Keywords: INDELs; endothelial cells; enrichment; genomic integrity; oncogenes; parental cells; pluripotent stem cells; point mutations; reprogramming; whole-genome sequencing
Mesh:
Year: 2021 PMID: 33831558 PMCID: PMC8353200 DOI: 10.1016/j.ymthe.2021.04.007
Source DB: PubMed Journal: Mol Ther ISSN: 1525-0016 Impact factor: 12.910