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首页> 外文期刊>Developmental biology >Myofibrillogenesis in the developing zebrafish heart: A functional study of tnnt2.
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Myofibrillogenesis in the developing zebrafish heart: A functional study of tnnt2.

机译:斑马鱼心脏发育中的肌原纤维形成:tnnt2的功能研究。

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摘要

Various hypotheses have been proposed to explain the molecule processes of sarcomere assembly, partially due to the lack of systematic genetic studies of sarcomeric genes in an in vivo model. Towards the goal of developing zebrafish as a vertebrate model for this purpose, we characterized myofibrillogenesis in a developing zebrafish heart and went on to examine the functions of cardiac troponin T (tnnt2). We found that sarcomere assembly in zebrafish heart was initiated from a non-striated actin filament network at the perimembrane region, whereas sarcomeric myosin is independently assembled into thick filaments of variable length before integrating into the thin filament network. Compared to Z-discs that are initially aligned to form shorter periodic dots and expanded longitudinally at a later time, M-lines assemble later and have a constant length. Depletion of full-length tnnt2 disrupted the striation of thin filaments and Z-bodies, which sequentially affects the striation of thick filaments and M-lines. Conversely, truncation of a C-terminal troponin complex-binding domain did not affect the striation of these sarcomere sub-structures, but resulted in reduced cardiomyocyte size. In summary, our data indicates that zebrafish are a valuable in vivo model for studying both myofibrillogenesis and sarcomere-based cardiac diseases.
机译:已经提出了各种假设来解释肌节组装的分子过程,部分原因是由于缺乏体内模型中肌节基因的系统遗传研究。为了实现将斑马鱼作为脊椎动物模型用于此目的,我们在斑马鱼心脏发育中表征了肌纤维形成,并进一步研究了心肌肌钙蛋白T(tnnt2)的功能。我们发现斑马鱼心脏中的肌节组装是由膜周围区域的非横纹肌动蛋白丝网络发起的,而肌节肌球蛋白在整合到细丝网络之前被独立组装成可变长度的粗丝。与最初对齐以形成较短的周期点并在以后纵向扩展的Z盘相比,M线稍后组装且具有恒定的长度。全长tnnt2的耗尽破坏了细丝和Z体的条纹,继而影响了粗丝和M线的条纹。相反,C-末端肌钙蛋白复合物结合结构域的截短不影响这些肌节亚结构的条纹,但导致心肌细胞大小减小。总而言之,我们的数据表明,斑马鱼是研究肌原纤维形成和基于肌节的心脏病的有价值的体内模型。

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