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Direct reprogramming of fibroblasts into cardiomyocytes

机译:将成纤维细胞直接重编程为心肌细胞

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Cardiovascular diseases are the leading causes of death in the world. The limited regenerative capacity of adult cardiomyocytes is the major barrier for heart regeneration. After myocardial infarction, myofibroblasts are the dominant cell type in the infarct zone. Therefore, it is a good idea to reprogram terminally differentiated myofibroblasts into cardiomyocyte-like cells directly, providing a good strategy to simultaneously reduce scar tissue and increase functional cardiomyocytes. Transcription factors were first identified to reprogram myofibroblasts into cardiomyocytes. Thereafter, microRNAs and/or small molecules showed great potential to optimize the reprogramming process. Here, we systemically summarize and compare the major progress in directed cardiac reprogramming including transcription factors and miRNAs, especially the small molecules. Furthermore, we discuss the challenges needed to be overcome to apply this strategy clinically.
机译:心血管疾病是世界上主要的死亡原因。成人心肌细胞的再生能力有限是心脏再生的主要障碍。心肌梗塞后,成肌纤维细胞是梗塞区的主要细胞类型。因此,将终末分化的成纤维细胞直接重编程为心肌样细胞是一个好主意,提供了同时减少疤痕组织和增加功能性心肌细胞的良好策略。首先鉴定出转录因子以将成肌纤维细胞重编程为心肌细胞。此后,microRNA和/或小分子显示出优化重新编程过程的巨大潜力。在这里,我们系统地总结和比较了定向心脏重编程的主要进展,包括转录因子和miRNA,尤其是小分子。此外,我们讨论了临床应用该策略需要克服的挑战。

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