首页> 美国卫生研究院文献>American Journal of Physiology - Gastrointestinal and Liver Physiology >Increased PDE5 activity and decreased Rho kinase and PKC activities in colonic muscle from caveolin-1−/− mice impair the peristaltic reflex and propulsion
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Increased PDE5 activity and decreased Rho kinase and PKC activities in colonic muscle from caveolin-1−/− mice impair the peristaltic reflex and propulsion

机译:Caveolin-1-/-小鼠结肠肌肉中PDE5活性增加Rho激酶和PKC活性降低削弱了蠕动反射和推进力

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摘要

Caveolae are specialized regions of the plasma membrane that concentrate receptors and associated signaling molecules critical in regulation of cellular response to transmitters and hormones. We have determined the effects of caveolin-1 (Cav-1) deletion, caveolin-1 siRNA, and caveolar disruption in mice on the signaling pathways that mediate contraction and relaxation in colonic smooth muscle and on the components of the peristaltic reflex in isolated tissue and propulsion in intact colonic segments. In Cav-1−/− mice, both relaxation and contraction were decreased in smooth muscle cells and muscle strips, as well as during both phases of the peristaltic reflex and colonic propulsion. The decrease in relaxation in response to the nitric oxide (NO) donor was accompanied by a decrease in cGMP levels and an increase in phosphodiesterase 5 (PDE5) activity. Relaxation by a PDE5-resistant cGMP analog was not affected in smooth muscle of Cav-1−/− mice, suggesting that inhibition of relaxation was due to augmentation of PDE5 activity. Similar effects on relaxation, PDE5 and cGMP were obtained in muscle cells upon disruption of caveolae by methyl-β-cyclodextrin or suppression of Cav-1. Sustained contraction mediated via inhibition of myosin light chain phosphatase (MLCP) activity is regulated by Rho kinase and PKC via phosphorylation of two endogenous inhibitors of MLCP: myosin phosphatase-targeting subunit (MYPT1) and 17-kDa PKC-potentiated protein phosphatase 1 inhibitor protein (CPI-17), respectively. The activity of both enzymes and phosphorylation of MYPT1 and CPI-17 were decreased in smooth muscle from Cav-1−/− mice. We conclude that the integrity of caveolae is essential for contractile and relaxant activity in colonic smooth muscle and the maintenance of neuromuscular function at organ level.
机译:小窝是质膜的专门区域,其集中在调节细胞对递质和激素反应中至关重要的受体和相关信号分子。我们已经确定了caveolin-1(Cav-1)缺失,caveolin-1 siRNA和小鼠海绵体破坏对介导结肠平滑肌收缩和松弛的信号通路以及离体组织的蠕动反射成分的影响和完整结肠段的推进。在Cav-1 -/-小鼠中,平滑肌细胞和肌肉条以及蠕动反射和结肠推进的两个阶段的松弛和收缩均降低。响应一氧化氮(NO)供体的弛豫的减少伴随着cGMP水平的降低和磷酸二酯酶5(PDE5)活性的增加。在Cav-1 -/-小鼠的平滑肌中,不受PDE5抗性的cGMP类似物的松弛作用不受影响,这表明松弛抑制作用是由于PDE5活性的增加所致。甲基-β-环糊精破坏小窝或抑制Cav-1后,对肌肉细胞的松弛,PDE5和cGMP的作用相似。 Rho激酶和PKC通过MLCP的两种内源性抑制剂的磷酸化来调节通过抑制肌球蛋白轻链磷酸酶(MLCP)活性介导的持续收缩:肌球蛋白磷酸酶靶向亚基(MYPT1)和17-kDa PKC增强蛋白磷酸酶1抑制剂蛋白(CPI-17)。 Cav-1 -/-小鼠的平滑肌中酶的活性以及MYPT1和CPI-17的磷酸化均降低。我们得出结论,小窝的完整性对于结肠平滑肌的收缩和松弛活动以及在器官水平上维持神经肌肉功能至关重要。

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