University Lille Nord de France, EA 4488, Laboratoire d'Activité Physique, Muscle et Santé, USTL, F-59655 Villeneuve d'Ascq, France.
Am J Physiol Regul Integr Comp Physiol. 2011 Feb;300(2):R408-17. doi: 10.1152/ajpregu.00793.2009. Epub 2010 Nov 24.
Our aim was to analyze the role of phosphatidylinositol 3-kinase (PI3K)-AKT and MAPK signaling pathways in the regulation of muscle mass and slow-to-fast phenotype transition during hindlimb unloading (HU). For that purpose, we studied, in rat slow soleus and fast extensor digitorum longus muscles, the time course of anabolic PI3K-AKT-mammalian target of rapamycin, catabolic PI3K-AKT-forkhead box O (FOXO), and MAPK signaling pathway activation after 7, 14, and 28 days of HU. Moreover, we performed chronic low-frequency soleus electrostimulation during HU to maintain exclusively contractile phenotype and so to determine more precisely the role of these signaling pathways in the modulation of muscle mass. HU induced a downregulation of the anabolic AKT, mammalian target of rapamycin, 70-kDa ribosomal protein S6 kinase, 4E-binding protein 1, and glycogen synthase kinase-3β targets, and an upregulation of the catabolic FOXO1 and muscle-specific RING finger protein-1 targets correlated with soleus muscle atrophy. Unexpectedly, soleus electrostimulation maintained 70-kDa ribosomal protein S6 kinase, 4E-binding protein 1, FOXO1, and muscle-specific RING finger protein-1 to control levels, but failed to reduce muscle atrophy. HU decreased ERK phosphorylation, while electrostimulation enabled the maintenance of ERK phosphorylation similar to control level. Moreover, slow-to-fast myosin heavy chain phenotype transition and upregulated glycolytic metabolism were prevented by soleus electrostimulation during HU. Taken together, our data demonstrated that the processes responsible for gradual disuse muscle plasticity in HU conditions involved both PI3-AKT and MAPK pathways. Moreover, electrostimulation during HU restored PI3K-AKT activation without counteracting soleus atrophy, suggesting the involvement of other signaling pathways. Finally, electrostimulation maintained initial contractile and metabolism properties in parallel to ERK activation, reinforcing the idea of a predominant role of ERK in the regulation of muscle slow phenotype.
我们的目的是分析磷脂酰肌醇 3-激酶 (PI3K)-AKT 和 MAPK 信号通路在下肢失用(HU)过程中调节肌肉质量和慢肌向快肌表型转变中的作用。为此,我们研究了在大鼠慢肌比目鱼肌和快肌趾长伸肌中,PI3K-AKT-雷帕霉素靶蛋白(mTOR)、PI3K-AKT-叉头框 O(FOXO)和 MAPK 信号通路在 HU 后 7、14 和 28 天的激活时间过程。此外,我们在 HU 期间对大鼠比目鱼肌进行慢性低频电刺激,以维持仅收缩表型,从而更准确地确定这些信号通路在调节肌肉质量中的作用。HU 导致合成代谢 AKT、mTOR、70kDa 核糖体蛋白 S6 激酶、4E 结合蛋白 1 和糖原合酶激酶-3β 靶标下调,以及分解代谢 FOXO1 和肌肉特异性 RING 指蛋白-1 靶标上调,与比目鱼肌萎缩相关。出乎意料的是,比目鱼肌电刺激维持了 70kDa 核糖体蛋白 S6 激酶、4E 结合蛋白 1、FOXO1 和肌肉特异性 RING 指蛋白-1 的对照水平,但未能减少肌肉萎缩。HU 降低了 ERK 磷酸化,而电刺激使 ERK 磷酸化维持在对照水平。此外,HU 期间比目鱼肌电刺激可防止快肌向慢肌肌球蛋白重链表型转变和糖酵解代谢的上调。总之,我们的数据表明,HU 条件下逐渐发生的废用性肌肉可塑性的过程涉及 PI3-AKT 和 MAPK 途径。此外,HU 期间的电刺激恢复了 PI3K-AKT 的激活,而没有对抗比目鱼肌萎缩,这表明其他信号通路的参与。最后,电刺激在平行于 ERK 激活的情况下维持了初始的收缩和代谢特性,这加强了 ERK 在调节肌肉慢表型中的主要作用的观点。
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