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High-Fidelity Reprogrammed Human IPSCs Have a High Efficacy of DNA Repair and Resemble hESCs in Their MYC Transcriptional Signature

机译:高保真重编程的人类IPSC具有MYC转录特征的DNA修复和类似于hESC的高效率。

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摘要

Human induced pluripotent stem cells (hiPSCs) are reprogrammed from adult or progenitor somatic cells and must make substantial adaptations to ensure genomic stability in order to become “embryonic stem cell- (ESC-) like.” The DNA damage response (DDR) is critical for maintenance of such genomic integrity. Herein, we determined whether cell of origin and reprogramming method influence the DDR of hiPSCs. We demonstrate that hiPSCs derived from cord blood (CB) myeloid progenitors (i.e., CB-iPSC) via an efficient high-fidelity stromal-activated (sa) method closely resembled hESCs in DNA repair gene expression signature and irradiation-induced DDR, relative to hiPSCs generated from CB or fibroblasts via standard methods. Furthermore, sa-CB-iPSCs also more closely resembled hESCs in accuracy of nonhomologous end joining (NHEJ), DNA double-strand break (DSB) repair, and C-MYC transcriptional signatures, relative to standard hiPSCs. Our data suggests that hiPSCs derived via more efficient reprogramming methods possess more hESC-like activated MYC signatures and DDR signaling. Thus, an authentic MYC molecular signature may serve as an important biomarker in characterizing the genomic integrity in hiPSCs.
机译:人类诱导的多能干细胞(hiPSC)从成年或祖细胞中重新编程,必须进行实质性适应以确保基因组稳定性,才能成为“胚胎干细胞(ESC-)样”。 DNA损伤反应(DDR)对于维持这种基因组完整性至关重要。在本文中,我们确定了起源单元和重编程方法是否会影响hiPSC的DDR。我们证明通过有效的高保真基质激活(sa)方法从脐带血(CB)髓样祖细胞(即CB-iPSC)衍生的hiPSC与DNA修复基因表达签名和辐射诱导DDR的hESC极为相似,相对于通过标准方法从炭黑或成纤维细胞中产生的hiPSC。此外,相对于标准hiPSC,sa-CB-iPSC在非同源末端连接(NHEJ),DNA双链断裂(DSB)修复和C-MYC转录特征的准确性上也更类似于hESC。我们的数据表明,通过更有效的重编程方法衍生的hiPSC具有更多的类似于hESC的活化MYC签名和DDR信号。因此,真实的MYC分子标记可以作为表征hiPSC中基因组完整性的重要生物标志物。

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