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Stem cells and reprogramming: breaking the epigenetic barrier?

机译:干细胞和重编程:打破表观遗传障碍?

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Increasing evidence suggests that epigenetic regulation is key to the maintenance of the stem cell state. Chromatin is the physiological form of eukaryotic genomes and the substrate for epigenetic marking, including DNA methylation, post-translational modifications of histones and the exchange of core histones with histone variants. The chromatin template undergoes significant reorganization during embryonic stem cell (ESC) differentiation and somatic cell reprogramming (SCR). Intriguingly, remodeling of the epigenome appears to be a crucial barrier that must be surmounted for efficient SCR. This area of research has gained significant attention due to the importance of ESCs in modeling and treating human disease. Here we review the epigenetic mechanisms that are key for maintenance of the ESC state, ESC differentiation and SCR. We focus on murine and human ESCs and induced pluripotent stem cells, and highlight the pharmacological approaches used to study or manipulate cell fate where relevant.
机译:越来越多的证据表明,表观遗传调控是维持干细胞状态的关键。染色质是真核生物基因组的生理形式,是表观遗传标记的底物,包括DNA甲基化,组蛋白的翻译后修饰以及核心组蛋白与组蛋白变体的交换。染色质模板在胚胎干细胞(ESC)分化和体细胞重编程(SCR)期间经历了重大重组。有趣的是,表观基因组的重塑似乎是有效SCR所必须克服的关键障碍。由于ESC在人类疾病的建模和治疗中的重要性,这一研究领域已引起了广泛的关注。在这里,我们回顾了表观遗传机制,这是维持ESC状态,ESC分化和SCR的关键。我们专注于鼠类和人类ESC和诱导性多能干细胞,并着重强调在相关时用于研究或操纵细胞命运的药理学方法。

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