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Modelling sarcomeric cardiomyopathies in the dish: from human heart samples to iPSC cardiomyocytes

机译:在培养皿中模拟肌节型心肌病:从人类心脏样本到iPSC心肌细胞

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摘要

One of the obstacles to a better understanding of the pathogenesis of human cardiomyopathies has been poor availability of heart-tissue samples at early stages of disease development. This has possibly changed by the advent of patient-derived induced pluripotent stem cell (hiPSC) from which cardiomyocytes can be derived in vitro. The main promise of hiPSC technology is that by capturing the effects of thousands of individual gene variants, the phenotype of differentiated derivatives of these cells will provide more information on a particular disease than simple genotyping. This article summarizes what is known about the 'human cardiomyopathy or heart failure phenotype in vitro', which constitutes the reference for modelling sarcomeric cardiomyopathies in hiPSC-derived cardiomyocytes. The current techniques for hiPSC generation and cardiac myocyte differentiation are briefly reviewed and the few published reports of hiPSC models of sarcomeric cardiomyopathies described. A discussion of promises and challenges of hiPSC-modelling of sarcomeric cardiomyopathies and individualized approaches is followed by a number of questions that, in the view of the authors, need to be answered before the true potential of this technology can be evaluated.
机译:更好地了解人类心肌病发病机制的障碍之一是在疾病发展的早期,心脏组织样本的可用性差。这可能是由于患者来源的诱导多能干细胞(hiPSC)的出现而改变的,心肌细胞可从该细胞中获得。 hiPSC技术的主要前景是,通过捕获成千上万的单个基因变体的作用,这些细胞的分化衍生物的表型将比简单的基因分型提供更多有关特定疾病的信息。本文总结了关于“体外人类心肌病或心力衰竭表型”的知识,这为在hiPSC来源的心肌细胞中建模肌节型心肌病提供了参考。简要回顾了hiPSC生成和心肌细胞分化的当前技术,并描述了肌节型心肌病的hiPSC模型的一些已发表的报道。在对结节性心肌病的hiPSC建模和个体化方法的前景和挑战进行讨论之后,作者认为,在评估该技术的真正潜力之前,需要回答一些问题。

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