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Beta-agonist drugs modulate the proliferation and differentiation of skeletal muscle cells

机译:β-激动剂药物调节骨骼肌细胞的增殖和分化

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摘要

Essentially employed for the treatment of airway obstructions in humans, β-agonists are also known to have an anabolic effect in animals’ skeletal muscle. In vivo and in vitro studies have attested the increase in animal body mass and the hypertrophy of muscle cells following the administration of specific β-agonists. However, the contribution of β-agonists to C2C12 myoblasts growth remains obscure. We therefore aimed to investigate the impact of β1-and β2-agonist drugs on the proliferation and differentiation of skeletal muscle cells. Direct observations and cytotoxicity assay showed that clenbuterol, salbutamol, cimaterol and ractopamine enhanced muscle cell growth and viability during the proliferation stage. Structural examinations coupled to Western blot analysis indicated that salbutamol and cimaterol triggered a decrease in myotube formation. A better comprehension of the effect of β-agonists on myogenic regulatory genes in the muscle cells is crucial to establish a specific role of β-agonists in muscle development, growth, and regeneration.
机译:基本上用于治疗人类的气道障碍物,β-激动剂也已知在动物的骨骼肌中具有合成代谢效应。体内和体外研究证明了在特定β-激动剂施用后的动物体重和肌肉细胞的肥大增加。然而,β-激动剂对C2C12肌细胞生长的贡献仍然模糊不清。因此,我们旨在探讨β1和β2激动剂药物对骨骼肌细胞增殖和分化的影响。直接观察和细胞毒性测定表明,在增殖阶段期间,Clenbuterol,Salbutamol,西莫米特和乳酰胺增强了肌肉细胞生长和活力。结合蛋白质印迹分析的结构考试表明,沙丁胺醇和西米物触发了肌管形成的降低。更好地理解β-激动剂对肌肉细胞中的肌原调控基因的影响对于建立β-激动剂在肌肉发育,生长和再生中的特定作用至关重要。

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