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通过大量肌肉特异性转录本的原位杂交显示的鱼类胚胎中的肌纤维分化。

Muscle fiber differentiation in fish embryos as shown by in situ hybridization of a large repertoire of muscle-specific transcripts.

作者信息

Chauvigné F, Cauty C, Rallière C, Rescan P Y

机构信息

Scribe-INRA, Campus de Beaulieu, 35042 Rennes, France.

出版信息

Dev Dyn. 2005 Jun;233(2):659-66. doi: 10.1002/dvdy.20371.

Abstract

Skeletal muscles are composed of different fiber types, largely defined by differential expression of protein isoforms involved in myofibrillogenesis or metabolism. To learn more about the gene activations that underlie the differentiation and the diversification of embryonic fish myotomal fibers, we investigated the developmental expression of 25 muscle genes in trout embryos by in situ hybridization of muscle-specific transcripts. The earliest event of muscle differentiation, at approximately the 25-somite stage, was the expression of a variety of muscle-specific genes, including slow-twitch and fast-twitch muscle isoforms. The activation of these muscle genes started in the deep somitic domain, where the slow muscle precursors (the adaxial cells) were initially located, and progressively spread laterally throughout the width of the myotome. This mediolateral progression of gene expression was coordinated with the lateral migration of slow adaxial cells, which specifically expressed the slow myosin light chain 1 and the SLIM1/FHL1 genes. Subsequently, the fast and slow skeletal muscle isoforms precociously expressed in the course of the mediolateral wave of muscle gene activation became down-regulated in the superficial slow fibers and the deep fast fibers, respectively. Finally, several muscle-specific genes, including troponins, a slow myosin-binding protein C, tropomodulins, and parvalbumin started their transcription only in late embryos. Taken together, these findings show in fish embryos that a common myogenic program is triggered in a mediolateral progression in all muscle cells. The acquisition of the slow phenotype involves the additional activation of several slow-specific genes in migrating adaxial muscle cells. These events are followed by sequential gene activations and repressions in fast and slow muscle cells.

摘要

骨骼肌由不同的纤维类型组成,主要由参与肌原纤维形成或代谢的蛋白质异构体的差异表达来定义。为了更多地了解胚胎鱼类肌节纤维分化和多样化背后的基因激活情况,我们通过肌肉特异性转录本的原位杂交研究了鳟鱼胚胎中25个肌肉基因的发育表达。肌肉分化的最早事件,大约在25体节阶段,是多种肌肉特异性基因的表达,包括慢肌和快肌异构体。这些肌肉基因的激活始于深部体节区域,慢肌前体细胞(轴旁细胞)最初位于此处,并逐渐横向扩散到整个肌节宽度。基因表达的这种中外侧进展与慢轴旁细胞的横向迁移相协调,这些细胞特异性表达慢肌球蛋白轻链1和SLIM1/FHL1基因。随后,在肌肉基因激活的中外侧波过程中早熟表达的快、慢骨骼肌异构体分别在浅表慢纤维和深部快纤维中下调。最后,包括肌钙蛋白、一种慢肌球蛋白结合蛋白C、原肌球蛋白和小清蛋白在内的几种肌肉特异性基因仅在晚期胚胎中开始转录。综上所述,这些发现表明在鱼类胚胎中,一个共同的成肌程序在所有肌肉细胞中以中外侧进展的方式被触发。慢表型的获得涉及迁移的轴旁肌肉细胞中几种慢特异性基因的额外激活。这些事件之后是快、慢肌肉细胞中基因的顺序激活和抑制。

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