Inhibition of desmin expression blocks myoblast fusion and interferes with the myogenic regulators MyoD and myogenin

结蛋白 MyoD公司 肌生成素 生物 肌发生 心肌细胞 融合蛋白 分子生物学 肌动蛋白 中间灯丝 细胞生物学 C2C12型 细胞 生物化学 细胞骨架 免疫学 基因 波形蛋白 重组DNA 免疫组织化学
作者
Hongmei Li,S. K. Choudhary,DJ Milner,MI Munir,IR Kuisk,Yassemi Capetanaki
出处
期刊:Journal of Cell Biology [Rockefeller University Press]
卷期号:124 (5): 827-841 被引量:163
标识
DOI:10.1083/jcb.124.5.827
摘要

The muscle-specific intermediate filament protein, desmin, is one of the earliest myogenic markers whose functional role during myogenic commitment and differentiation is unknown. Sequence comparison of the presently isolated and fully characterized mouse desmin cDNA clones revealed a single domain of polypeptide similarity between desmin and the basic and helix-loop-helix region of members of the myoD family myogenic regulators. This further substantiated the need to search for the function of desmin. Constructs designed to express anti-sense desmin RNA were used to obtain stably transfected C2C12 myoblast cell lines. Several lines were obtained where expression of the anti-sense desmin RNA inhibited the expression of desmin RNA and protein down to basal levels. As a consequence, the differentiation of these myoblasts was blocked; complete inhibition of myoblast fusion and myotube formation was observed. Rescue of the normal phenotype was achieved either by spontaneous revertants, or by overexpression of the desmin sense RNA in the defective cell lines. In several of the cell lines obtained, inhibition of desmin expression was followed by differential inhibition of the myogenic regulators myoD and/or myogenin, depending on the stage and extent of desmin inhibition in these cells. These data suggested that myogenesis is modulated by at least more than one pathway and desmin, which so far was believed to be merely an architectural protein, seems to play a key role in this process.
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