Desgeorges Marine Maud, Devillard Xavier, Toutain Jérome, Divoux Didier, Castells Josiane, Bernaudin Myriam, Touzani Omar, Freyssenet Damien Gilles
From the Laboratoire de Physiologie de l'Exercice, Université de Lyon, Saint Etienne, France (M.M.D., X.D., J.C., D.G.F.); CNRS, UMR 6301 ISTCT, CERVOxy Group, GIP Cyceron, Caen, France (J.T., D.D., M.B., O.T.); CEA, DSV/I2BM, UMR 6301 ISTCT, Caen, France (J.T., D.D., M.B., O.T.); and Université de Caen Basse Normandie, UMR 6301 ISTCT, Caen, France (J.T., D.D., M.B., O.T.).
Stroke. 2015 Jun;46(6):1673-80. doi: 10.1161/STROKEAHA.114.008574. Epub 2015 May 7.
Loss of muscle mass and function is a severe complication in patients with stroke that contributes to promoting physical inactivity and disability. The deleterious consequences of skeletal muscle mass loss underline the necessity to identity the molecular mechanisms involved in skeletal muscle atrophy after cerebral ischemia.
Transient focal cerebral ischemia (60 minutes) was induced by occlusion of the right middle cerebral artery in C57BL/6J male mice. Skeletal muscles were removed 3 days later and analyzed for the regulation of critical determinants of muscle mass homeostasis (Akt/mammalian target of rapamycin pathway, myostatin-Smad2/3 and bone morphogenetic protein-Smad1/5/8 signaling pathways, ubiquitin-proteasome and autophagy-lysosome proteolytic pathways).
Cerebral ischemia induced severe sensorimotor deficits associated with muscle mass loss of the paretic limbs. Mechanistically, cerebral ischemia repressed Akt/mammalian target of rapamycin pathway and increased expression of key players of ubiquitin-proteasome pathway (MuRF1 [muscle RING finger-1], MAFbx [muscle atrophy F-box], Musa1 [muscle ubiquitin ligase of SCF complex in atrophy-1]), together with a marked increase in myostatin expression, in both paretic and nonparetic skeletal muscles. The Smad1/5/8 pathway was also activated.
Our data fit with a model in which a repression of Akt/mammalian target of rapamycin pathway and an increase in the expression of key players of ubiquitin-proteasome pathway are critically involved in skeletal muscle atrophy after cerebral ischemia. Cerebral ischemia also caused an activation of bone morphogenetic protein-Smad1/5/8 signaling pathway, suggesting that compensatory mechanisms are also concomitantly activated to limit the extent of skeletal muscle atrophy.
肌肉质量和功能丧失是中风患者的一种严重并发症,会促使身体活动减少和残疾。骨骼肌质量丧失的有害后果突显了确定脑缺血后骨骼肌萎缩所涉及分子机制的必要性。
通过阻断C57BL/6J雄性小鼠的右侧大脑中动脉诱导短暂性局灶性脑缺血(60分钟)。3天后取出骨骼肌,分析肌肉质量稳态关键决定因素的调节情况(Akt/雷帕霉素哺乳动物靶标途径、肌肉生长抑制素-Smad2/3和骨形态发生蛋白-Smad1/5/8信号通路、泛素-蛋白酶体和自噬-溶酶体蛋白水解途径)。
脑缺血导致严重的感觉运动功能障碍,伴有瘫痪肢体的肌肉质量丧失。从机制上讲,脑缺血抑制了Akt/雷帕霉素哺乳动物靶标途径,增加了泛素-蛋白酶体途径关键因子(MuRF1 [肌肉环指蛋白-1]、MAFbx [肌肉萎缩F盒蛋白]、Musa1 [萎缩-1中SCF复合物的肌肉泛素连接酶])的表达,同时在瘫痪和未瘫痪的骨骼肌中肌肉生长抑制素表达显著增加。Smad1/5/8途径也被激活。
我们的数据符合一种模型,即Akt/雷帕霉素哺乳动物靶标途径的抑制和泛素-蛋白酶体途径关键因子表达的增加在脑缺血后骨骼肌萎缩中起关键作用。脑缺血还导致骨形态发生蛋白-Smad1/5/8信号通路的激活,表明补偿机制也同时被激活以限制骨骼肌萎缩的程度。
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