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Reprogramming human peripheral blood mononuclear cells to inducible pluripotent stem cells (hiPSC): An examination of the efficacy of different methods

机译:将人外周血单核细胞重编程为诱导性多能干细胞(hiPSC):检查不同方法的功效

摘要

Modeling a disease “in a dish,” a new research tool to study human heart disease mechanisms, is becoming as popular as more established techniques such as the use of transgenic mice. The primary practical challenge of this “disease in a dish” method is efficiently directing human induced pluripotent stem cell (hiPSC) differentiation into the desired lineages, with the major concern being the variability within hiPSC clones.To generate a reliable in vitro model for inherited cardiac diseases and address the variability problem, characteristics of hiPSCs derived from the blood of four human donors using both the episomal and Sendai virus reprogramming systems were examined. The hiPSC-cardiomyocytes (hiPSC-CMs) generated were then characterized according to their cardiac-specific gene expression properties. No differences were observed on the effect of the reprogramming system on expression of pluripotent genes in iPSCs but differences were observed in expression of cardiac specific genes in cardiomyocytes derived from those iPSCs despite a high variance in the analysis.
机译:一种“盘中”疾病的模型,一种研究人类心脏病机理的新研究工具,已经与更成熟的技术(例如使用转基因小鼠)一样流行。这种“一碟中的疾病”方法的主要实际挑战是有效地将人类诱导的多能干细胞(hiPSC)分化引导到所需的谱系中,其中主要的问题是hiPSC克隆内的变异性。生成可靠的体外遗传模型心脏疾病并解决变异性问题,研究了使用附加型和仙台病毒重编程系统从四个人类供体血液中提取的hiPSC的特征。然后根据它们的心脏特异性基因表达特性对产生的hiPSC-心肌细胞(hiPSC-CM)进行表征。在重编程系统对iPSC中多能基因表达的影响方面未观察到差异,但是尽管分析差异很大,但在衍生自这些iPSC的心肌细胞中心脏特异性基因的表达中未观察到差异。

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    Afshinmanesh Elham;

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  • 年度 2016
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