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细胞融合在斑马鱼胚胎后发育的慢肌和快肌中受到差异调控。

Cell fusion is differentially regulated in zebrafish post-embryonic slow and fast muscle.

机构信息

Department of Molecular Genetics and Biological Chemistry and Pharmacology, The Ohio State University, Columbus, OH, 43210, USA; Center for Muscle Health and Neuromuscular Disorders, The Ohio State University and Nationwide Children's Hospital, Columbus, OH, 43210, USA; Molecular, Cellular, and Developmental Biology Graduate Program, The Ohio State University, Columbus, OH, 43210, USA.

Department of Molecular Genetics and Biological Chemistry and Pharmacology, The Ohio State University, Columbus, OH, 43210, USA; Center for Muscle Health and Neuromuscular Disorders, The Ohio State University and Nationwide Children's Hospital, Columbus, OH, 43210, USA.

出版信息

Dev Biol. 2020 Jun 1;462(1):85-100. doi: 10.1016/j.ydbio.2020.03.005. Epub 2020 Mar 10.

Abstract

Skeletal muscle fusion occurs during development, growth, and regeneration. To investigate how muscle fusion compares among different muscle cell types and developmental stages, we studied muscle cell fusion over time in wild-type, myomaker (mymk), and jam2a mutant zebrafish. Using live imaging, we show that embryonic myoblast elongation and fusion correlate tightly with slow muscle cell migration. In wild-type embryos, only fast muscle fibers are multinucleate, consistent with previous work showing that the cell fusion regulator gene mymk is specifically expressed throughout the embryonic fast muscle domain. However, by 3 weeks post-fertilization, slow muscle fibers also become multinucleate. At this late-larval stage, mymk is not expressed in muscle fibers, but is expressed in small cells near muscle fibers. Although previous work showed that both mymk and jam2a are required for embryonic fast muscle cell fusion, we observe that muscle force and function is almost normal in mymk and jam2a mutant embryos, despite the lack of fast muscle multinucleation. We show that genetic requirements change post-embryonically, with jam2a becoming much less important by late-larval stages and mymk now required for muscle fusion and growth in both fast and slow muscle cell types. Correspondingly, adult mymk mutants perform poorly in sprint and endurance tests compared to wild-type and jam2a mutants. We show that adult mymk mutant muscle contains small mononucleate myofibers with average myonuclear domain size equivalent to that in wild type adults. The mymk mutant fibers have decreased Laminin expression and increased numbers of Pax7-positive cells, suggesting that impaired fiber growth and active regeneration contribute to the muscle phenotype. Our findings identify several aspects of muscle fusion that change with time in slow and fast fibers as zebrafish develop beyond embryonic stages.

摘要

骨骼肌融合发生在发育、生长和再生过程中。为了研究不同类型的肌肉细胞和发育阶段的肌肉融合情况,我们研究了野生型、myomaker(mymk)和 jam2a 突变体斑马鱼中肌肉细胞随时间的融合情况。通过活体成像,我们发现胚胎期肌细胞的伸长和融合与慢肌细胞的迁移密切相关。在野生型胚胎中,只有快肌纤维是多核的,这与之前的工作一致,表明细胞融合调节基因 mymk 在整个胚胎快肌域中特异性表达。然而,到受精后 3 周,慢肌纤维也变成多核的。在这个晚期幼虫阶段,mymk 不在肌肉纤维中表达,而是在肌肉纤维附近的小细胞中表达。尽管之前的研究表明 mymk 和 jam2a 都需要胚胎期快肌细胞融合,但我们观察到,尽管缺乏快肌多核化,mymk 和 jam2a 突变体胚胎的肌肉力量和功能几乎正常。我们表明,遗传需求在胚胎后发生变化,jam2a 在晚期幼虫阶段变得不那么重要,而 mymk 现在对于快肌和慢肌细胞类型的肌肉融合和生长都是必需的。相应地,与野生型和 jam2a 突变体相比,成年 mymk 突变体在短跑和耐力测试中表现不佳。我们表明,成年 mymk 突变体肌肉包含小的单核肌纤维,其平均肌核域大小与野生型成年鱼相当。mymk 突变体纤维的层粘连蛋白表达减少,Pax7 阳性细胞增多,表明受损的纤维生长和活跃的再生导致了肌肉表型。我们的研究结果确定了在斑马鱼发育到胚胎阶段之后,慢肌和快肌纤维随时间变化的几个肌肉融合方面。

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