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Abnormalities of satellite cells function in amyotrophic lateral sclerosis

机译:卫星细胞异常在肌萎缩性侧索硬化中的功能

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摘要

Amyotrophic lateral sclerosis (ALS) is characterized by progressive denervation leading to muscle atrophy prevented, during the early phase, by compensatory reinnervation. Little is known about muscle fibre regeneration capacity in ALS. We have carried out in vivo and in vitro investigation of skeletal muscle in ALS. Seven ALS patients underwent a deltoid muscle biopsy. Immunohistochemical analysis revealed various degrees of denervation- and reinnervation-related changes in the ALS muscle biopsies including satellite cells (SCs) activation and regenerating fibres. Only 3/7 primary cultures of ALS muscle cells were successfully established and had sufficient myogenicity, as assessed by desmin positivity, to be used without further purification. This was in contrast with the cultures derived from control muscles, predominantly desmin-positive cells. Although capable to proliferate in vitro, ALS-derived SCs presented an abnormal senescent-like morphology. Markers of senescence, including senescent-associated (SA)-βGal activity and p16 expression, were increased. Furthermore, ALS-derived SCs were also unable to fully differentiate in vitro as shown by abnormal myotubes morphology and reduced MHC isoform expression, compared to control myotubes. Our study suggests that SC function is altered in ALS. This could limit the efficacy of compensatory processes and therefore could contribute to the progression of muscle atrophy and weakness.
机译:肌萎缩性侧索硬化症(ALS)的特征是进行性去神经支配,导致在早期通过代偿性神经支配来预防肌肉萎缩。关于ALS中的肌纤维再生能力知之甚少。我们已经对ALS中的骨骼肌进行了体内和体外研究。 7名ALS患者接受了三角肌活检。免疫组织化学分析揭示了ALS肌肉活检中与神经支配和神经支配相关的各种变化,包括卫星细胞(SCs)激活和再生纤维。仅成功建立了ALS肌肉细胞的3/7原代培养物,并且具有足够的成肌能力(通过结蛋白阳性评估),无需进一步纯化即可使用。这与源自对照肌肉,主要是结蛋白阳性细胞的培养物形成对比。尽管能够在体外增殖,但ALS衍生的SC呈现出异常的衰老样形态。衰老的标志物,包括衰老相关的(SA)-βGal活性和p16表达增加。此外,与正常肌管相比,异常肌管形态和MHC亚型表达降低表明,ALS衍生的SC不能在体外完全分化。我们的研究表明,ALS中的SC功能有所改变。这可能会限制代偿过程的功效,因此可能导致肌肉萎缩和无力的进展。

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