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肌营养不良小鼠(mdx和dy)再生过程中MyoD和生肌调节因子的表达。

Expression of MyoD and myogenin in dystrophic mice, mdx and dy, during regeneration.

作者信息

Jin Y, Murakami N, Saito Y, Goto Y, Koishi K, Nonaka I

机构信息

Department of Ultrastructural Research, National Center of Neurology and Psychiatry (NCNP), Tokyo, Japan.

出版信息

Acta Neuropathol. 2000 Jun;99(6):619-27. doi: 10.1007/s004010051172.

Abstract

Expression of two myogenic regulatory factors, MyoD and myogenin, was studied in regenerating muscles of dystrophic mice and compared to a chemically induced regeneration process. First, the distribution of the two proteins was determined immunohistochemically at various time points after single administrations of a local anaesthetic, bupivacaine hydrochloride, which causes myonecrosis followed by regeneration. Detectable levels of MyoD appeared at 18 h and the expression reached their maximum levels at 48 h after the injection, which coincide with the stage when satellite cells are activated and start to proliferate. Myogenin became detectable in 24 h and its expression reached its highest level at 72 h after injection when newly formed myotubes appeared. The two genes were also expressed in the dystrophic muscles from dy and mdx mice which exhibit dystrophic pathological features but are associated with different phenotypes. In mdx mice the two genes were expressed at reasonably high levels in parallel with the active regenerating process, whereas in dy mice MyoD and myogenin expressions decreased as fibrosis progressed. However, MyoD was relatively more strongly expressed in the larger mature myotubes of dy mice than in those of mdx mice, suggesting prolonged regenerative activity. In dy and mdx mice, MyoD and myogenin were expressed in different quantities, indicating that these animals have distinct regenerating activities. Our findings confirm that expression of both MyoD and myogenin genes is necessary in the regenerative process for the proliferation of satellite cells (myoblasts) and for the development of early regenerating fibers (myotubes) even in dystrophic muscles.

摘要

在营养不良小鼠的再生肌肉中研究了两种生肌调节因子MyoD和肌细胞生成素的表达,并与化学诱导的再生过程进行了比较。首先,在单次给予局部麻醉剂盐酸布比卡因后,通过免疫组织化学方法在不同时间点确定这两种蛋白质的分布,盐酸布比卡因会导致肌坏死随后再生。注射后18小时可检测到MyoD水平,其表达在注射后48小时达到最高水平,这与卫星细胞被激活并开始增殖的阶段一致。肌细胞生成素在24小时时可被检测到,其表达在注射后72小时新形成肌管时达到最高水平。这两个基因也在表现出营养不良病理特征但与不同表型相关的dy和mdx小鼠的营养不良肌肉中表达。在mdx小鼠中,这两个基因在活跃的再生过程中以相当高的水平表达,而在dy小鼠中,随着纤维化进展,MyoD和肌细胞生成素的表达下降。然而,MyoD在dy小鼠较大的成熟肌管中表达相对比mdx小鼠更强,表明再生活动持续时间更长。在dy和mdx小鼠中,MyoD和肌细胞生成素的表达量不同,表明这些动物具有不同的再生活动。我们的研究结果证实,即使在营养不良肌肉中,MyoD和肌细胞生成素基因的表达对于卫星细胞(成肌细胞)的增殖以及早期再生纤维(肌管)的发育在再生过程中都是必需的。

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