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Human pluripotent stem cell-derived cardiomyocytes for heart regeneration, drug discovery and disease modeling: from the genetic, epigenetic, and tissue modeling perspectives

机译:人类多能干细胞衍生的心肌细胞用于心脏再生,药物发现和疾病建模:从遗传,表观遗传学和组织建模的角度

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Heart diseases remain a major cause of mortality and morbidity worldwide. However, terminally differentiated human adult cardiomyocytes (CMs) possess a very limited innate ability to regenerate. Directed differentiation of human embryonic stem cells (hESCs) and induced pluripotent stem cells (iPSCs) into CMs has enabled clinicians and researchers to pursue the novel therapeutic paradigm of cell-based cardiac regeneration. In addition to tissue engineering and transplantation studies, the need for functional CMs has also prompted researchers to explore molecular pathways and develop strategies to improve the quality, purity and quantity of hESC-derived and iPSC-derived CMs. In this review, we describe various approaches in directed CM differentiation and driven maturation, and discuss potential limitations associated with hESCs and iPSCs, with an emphasis on the role of epigenetic regulation and chromatin remodeling, in the context of the potential and challenges of using hESC-CMs and iPSC-CMs for drug discovery and toxicity screening, disease modeling, and clinical applications.
机译:心脏病仍然是全世界死亡率和发病率的主要原因。然而,终末分化的人类成年心肌细胞(CMs)具有非常有限的先天再生能力。人类胚胎干细胞(hESCs)和诱导性多能干细胞(iPSCs)定向定向分化为CM,使临床医生和研究人员能够追求基于细胞的心脏再生的新型治疗范例。除组织工程和移植研究外,对功能性CM的需求还促使研究人员探索分子途径,并制定策略来改善hESC衍生和iPSC衍生CM的质量,纯度和数量。在这篇综述中,我们描述了定向CM分化和驱动成熟的各种方法,并讨论了与hESC和iPSC相关的潜在限制,重点是在使用hESC的潜力和挑战的背景下,表观遗传调控和染色质重塑的作用。 -CM和iPSC-CM用于药物发现和毒性筛选,疾病建模和临床应用。

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