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首页> 外文期刊>Nature Communications >Tbx5a lineage tracing shows cardiomyocyte plasticity during zebrafish heart regeneration
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Tbx5a lineage tracing shows cardiomyocyte plasticity during zebrafish heart regeneration

机译:Tbx5a谱系追踪显示斑马鱼心脏再生过程中的心肌细胞可塑性

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摘要

During development, mesodermal progenitors from the first heart field (FHF) form a primitive cardiac tube, to which progenitors from the second heart field (SHF) are added. The contribution of FHF and SHF progenitors to the adult zebrafish heart has not been studied to date. Here we find, using genetic tbx5a lineage tracing tools, that the ventricular myocardium in the adult zebrafish is mainly derived from tbx5a+ cells, with a small contribution from tbx5a? SHF progenitors. Notably, ablation of ventricular tbx5a+-derived cardiomyocytes in the embryo is compensated by expansion of SHF-derived cells. In the adult, tbx5a expression is restricted to the trabeculae and excluded from the outer cortical layer. tbx5a-lineage tracing revealed that trabecular cardiomyocytes can switch their fate and differentiate into cortical myocardium during adult heart regeneration. We conclude that a high degree of cardiomyocyte cell fate plasticity contributes to efficient regeneration.
机译:在发育过程中,来自第一个心脏区域(FHF)的中胚层祖细胞形成原始的心管,并向其中添加了来自第二个心脏区域(SHF)的祖细胞。迄今为止,尚未研究FHF和SHF祖细胞对成年斑马鱼心脏的贡献。在这里,我们发现使用遗传性tbx5a谱系追踪工具,成年斑马鱼的心室心肌主要来源于tbx5a +细胞,而tbx5a贡献很小? SHF祖细胞。值得注意的是,胚胎中心室tbx5a +衍生的心肌细胞的消融可通过SHF衍生的细胞的扩增来补偿。在成年人中,tbx5a的表达仅限于小梁,并被排除在皮层外层。 tbx5a谱系追踪显示,在成年心脏再生过程中,小梁型心肌细胞可以改变命运,并分化为皮层心肌。我们得出结论,高度的心肌细胞命运可塑性有助于有效的再生。

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