蛋白酶激活受体在灵长类结肠肌肉中通过激活钙敏化途径对收缩反应的功能作用。
The functional role of protease-activated receptors on contractile responses by activation of Ca sensitization pathways in simian colonic muscles.
机构信息
Department of Physiology and Cell Biology, University of Nevada School of Medicine , Reno, Nevada.
Department of Physiology, School of Medicine, Shanghai Jiao Tong University , Shanghai , China.
出版信息
Am J Physiol Gastrointest Liver Physiol. 2018 Dec 1;315(6):G921-G931. doi: 10.1152/ajpgi.00255.2018. Epub 2018 Sep 27.
It has been known that activation of protease-activated receptors (PARs) affects gastrointestinal motility. In this study, we tested the effects of PAR agonists on electrical and contractile responses and Ca sensitization pathways in simian colonic muscles. The Simian colonic muscle was initially hyperpolarized by PAR agonists. After the transient hyperpolarization, simian colonic muscle repolarized to the control resting membrane potential (RMP) without a delayed depolarization. Apamin significantly reduced the initial hyperpolarization, suggesting that activation of small conductance Ca-activated K (SK) channels is involved in the initial hyperpolarization. In contractile experiments, PAR agonists caused an initial relaxation followed by an increase in contractions. These delayed contractile responses were not matched with the electrical responses that showed no after depolarization of the RMP. To investigate the possible involvement of Rho-associated protein kinase 2 (ROCK) pathways in the PAR effects, muscle strips were treated with ROCK inhibitors, which significantly reduced the PAR agonist-induced contractions. Furthermore, PAR agonists increased MYPT1 phosphorylation, and ROCK inhibitors completely blocked MYPT1 phosphorylation. PAR agonists alone had no effect on CPI-17 phosphorylation. In the presence of apamin, PAR agonists significantly increased CPI-17 phosphorylation, which was blocked by protein kinase C (PKC) inhibitors suggesting that Ca influx is increased by apamin and is activating PKC. In conclusion, these studies show that PAR activators induce biphasic responses in simian colonic muscles. The initial inhibitory responses by PAR agonists are mainly mediated by activation of SK channels and delayed contractile responses are mainly mediated by the CPI-17 and ROCK Ca sensitization pathways in simian colonic muscles. NEW & NOTEWORTHY In the present study, we found that the contractile responses of simian colonic muscles to protease-activated receptor (PAR) agonists are different from the previously reported contractile responses of murine colonic muscles. Ca sensitization pathways mediate the contractile responses of simian colonic muscles to PAR agonists without affecting the membrane potential. These findings emphasize novel mechanisms of PAR agonist-induced contractions possibly related to colonic dysmotility in inflammatory bowel disease.
已经知道蛋白酶激活受体 (PARs) 的激活会影响胃肠道蠕动。在这项研究中,我们测试了 PAR 激动剂对灵长类结肠肌肉的电和收缩反应以及钙敏化途径的影响。PAR 激动剂最初使灵长类结肠肌肉超极化。在短暂的超极化之后,灵长类结肠肌肉重新极化到对照静息膜电位 (RMP),没有延迟去极化。阿帕米因显著减少了初始超极化,表明小电导钙激活钾 (SK) 通道的激活参与了初始超极化。在收缩实验中,PAR 激动剂引起初始松弛,随后收缩增加。这些延迟的收缩反应与没有 RMP 后去极化的电反应不匹配。为了研究 Rho 相关蛋白激酶 2 (ROCK) 途径在 PAR 作用中的可能参与,用 ROCK 抑制剂处理肌肉条带,这显著减少了 PAR 激动剂诱导的收缩。此外,PAR 激动剂增加了 MYPT1 磷酸化,而 ROCK 抑制剂完全阻断了 MYPT1 磷酸化。PAR 激动剂单独对 CPI-17 磷酸化没有影响。在阿帕米因存在的情况下,PAR 激动剂显著增加了 CPI-17 的磷酸化,这被蛋白激酶 C (PKC) 抑制剂阻断,表明钙内流增加是通过阿帕米因激活 PKC 引起的。总之,这些研究表明,PAR 激活剂在灵长类结肠肌肉中诱导双相反应。PAR 激动剂的初始抑制反应主要由 SK 通道的激活介导,而延迟的收缩反应主要由 CPI-17 和 ROCK 钙敏化途径介导。
在本研究中,我们发现灵长类结肠肌肉对蛋白酶激活受体 (PAR) 激动剂的收缩反应与先前报道的鼠结肠肌肉的收缩反应不同。钙敏化途径介导灵长类结肠肌肉对 PAR 激动剂的收缩反应,而不影响膜电位。这些发现强调了 PAR 激动剂诱导收缩的新机制,可能与炎症性肠病中的结肠运动障碍有关。
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