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Muscle sparing in muscle RING finger 1 null mice: response to synthetic glucocorticoids

机译:肌肉无名指1号空小鼠的肌肉备用:对合成糖皮质激素的反应

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摘要

Non-technical summarySkeletal muscle has the capacity to modify its size in response to external cues such as mechanical load, neural activity, hormones, stress and nutritional status. Pathological muscle loss or ‘atrophy’ occurs as the result of a number of disparate conditions including ageing, immobilization, diabetes, cancer, sepsis and as a serious side effect of corticosteroid hormone treatment. Synthetic glucocorticoids are often used to treat inflammation; however, high doses and chronic use of these hormones can lead to the loss of skeletal muscle mass and weakness. We show that in mice with a deletion of the MuRF1 protein, but not the MAFbx protein, the loss of muscle mass is attenuated relative to normal mice following 14 days of glucocorticoid treatment. Knowledge of how the MuRF1 protein functions in skeletal muscle to regulate skeletal muscle mass could lead to the development of therapeutics to prevent muscle atrophy under various conditions including glucocorticoid treatment.
机译:非技术性总结骨骼肌具有根据外部提示(例如机械负荷,神经活动,激素,压力和营养状况)改变自身大小的能力。病理性肌肉丢失或“萎缩”是由于多种不同的状况而导致的,包括衰老,固定,糖尿病,癌症,败血症以及皮质类固醇激素治疗的严重副作用。合成的糖皮质激素常用于治疗炎症。但是,高剂量和长期使用这些激素会导致骨骼肌质量下降和虚弱。我们显示,在删除MuRF1蛋白而不是MAFbx蛋白的小鼠中,糖皮质激素治疗14天后,肌肉质量的损失相对于正常小鼠而言有所减弱。关于MuRF1蛋白如何在骨骼肌中调节骨骼肌质量的知识可能会导致开发预防包括糖皮质激素在内的各种条件下的肌肉萎缩的疗法。

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