| Literature DB >> 33589441 |
Minglin Ou1,2, Min Zhao3, Chunhong Li4,5, Donge Tang2, Yong Xu2, Weier Dai6, Weiguo Sui4, Yue Zhang4, Zhen Xiang4, Chune Mo4, Hua Lin4, Yong Dai7,4.
Abstract
Human induced pluripotent stem cells (iPSCs) are important source for regenerative medicine. However, the links between pluripotency and oncogenic transformation raise safety issues. To understand the characteristics of iPSC-derived cells at single-cell resolution, we directly reprogrammed two human iPSC lines into cardiomyocytes and collected cells from four time points during cardiac differentiation for single-cell sequencing. We captured 32,365 cells and identified five molecularly distinct clusters that aligned well with our reconstructed differentiation trajectory. We discovered a set of dynamic expression events related to the upregulation of oncogenes and the decreasing expression of tumor suppressor genes during cardiac differentiation, which were similar to the gain-of-function and loss-of-function patterns during oncogenesis. In practice, we characterized the dynamic expression of the TP53 and Yamanaka factor genes (OCT4, SOX2, KLF4 and MYC), which were widely used for human iPSCs lines generation; and revealed the co-occurrence of MYC overexpression and TP53 silencing in some of human iPSC-derived TNNT2+ cardiomyocytes. In summary, our oncogenic expression atlas is valuable for human iPSCs application and the single-cell resolution highlights the clues potentially associated with the carcinogenic risk of human iPSC-derived cells.Entities:
Keywords: MYC; Oncogene; Single-cell transcriptomics; TP53; Tumor suppressor gene
Mesh:
Year: 2021 PMID: 33589441 PMCID: PMC7903994 DOI: 10.1242/bio.053348
Source DB: PubMed Journal: Biol Open ISSN: 2046-6390 Impact factor: 2.422