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Expression analysis of Baf60c during heart regeneration in axolotls and neonatal mice

机译:Baf60c在x和新生小鼠心脏再生过程中的表达分析

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Some organisms, such as zebrafish, urodele amphibians, and newborn mice, have a capacity for heart regeneration following injury. However, adult mammals fail to regenerate their hearts. To know why newborn mice can regenerate their hearts, we focused on epigenetic factors, which are involved in cell differentiation in many tissues. Baf60c (BRG1/BRM-associated factor 60c), a component of ATP-dependent chromatin-remodeling complexes, has an essential role for cardiomyocyte differentiation at the early heart development. To address the function of Baf60c in postnatal heart homeostasis and regeneration, we examined the detailed expression/localization patterns of Baf60c in both mice and axolotls. In the mouse heart development, Baf60c was highly expressed in the entire heart at the early stages, but gradually downregulated at the postnatal stages. During heart regeneration in neonatal mice and axolotls, Baf60c expression was strongly upregulated after resection. Interestingly, the timing of Baf60c upregulation after resection was consistent with the temporal dynamics of cardiomyocyte proliferation. Moreover, knockdown of Baf60c downregulated proliferation of neonatal mouse cardiomyocytes. These data suggested that Baf60c plays an important role in cardiomyocyte proliferation in heart development and regeneration. This is the first study indicating that Baf60c contributes to the heart regeneration in vertebrates.
机译:某些生物(例如斑马鱼,两栖类urodele和新生小鼠)具有受伤后心脏再生的能力。但是,成年哺乳动物无法使其心脏再生。要了解新生小鼠为何能够再生其心脏,我们集中于表观遗传因子,后者与许多组织的细胞分化有关。 Baf60c(BRG1 / BRM相关因子60c)是ATP依赖的染色质重塑复合物的组成部分,在心脏早期发育中对心肌细胞的分化具有重要作用。为了解决Baf60c在产后心脏动态平衡和再生中的功能,我们检查了Baf60c在小鼠和轴突中的详细表达/定位模式。在小鼠心脏发育中,Baf60c在早期阶段在整个心脏中高度表达,但在产后阶段逐渐下调。在新生小鼠和a的心脏再生过程中,Baf60c表达在切除后强烈上调。有趣的是,切除后Baf60c上调的时机与心肌细胞增殖的时间动态一致。此外,Baf60c的敲低下调了新生小鼠心肌细胞的增殖。这些数据表明Baf60c在心脏发育和再生中的心肌细胞增殖中起重要作用。这是第一项表明Baf60c有助于脊椎动物心脏再生的研究。

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