Joshi Shreena, Balan Prabhu, Gurney Alison M
Department of Physiology & Pharmacology, University of Strathclyde, Glasgow G4 0NR, UK.
Respir Res. 2006 Feb 20;7(1):31. doi: 10.1186/1465-9921-7-31.
KCNQ channels have been widely studied in the nervous system, heart and inner ear, where they have important physiological functions. Recent reports indicate that KCNQ channels may also be expressed in portal vein where they are suggested to influence spontaneous contractile activity. The biophysical properties of K+ currents mediated by KCNQ channels resemble a current underlying the resting K+ conductance and resting potential of pulmonary artery smooth muscle cells. We therefore investigated a possible role of KCNQ channels in regulating the function of pulmonary arteries by determining the ability of the selective KCNQ channel blockers, linopirdine and XE991, to promote pulmonary vasoconstriction.
The tension developed by rat and mouse intrapulmonary or mesenteric arteries was measured using small vessel myography. Contractile responses to linopirdine and XE991 were measured in intact and endothelium denuded vessels. Experiments were also carried out under conditions that prevent the contractile effects of nerve released noradrenaline or ATP, or block various Ca2+ influx pathways, in order to investigate the mechanisms underlying contraction.
Linopirdine and XE991 both contracted rat and mouse pulmonary arteries but had little effect on mesenteric arteries. In each case the maximum contraction was almost as large as the response to 50 mM K+. Linopirdine had an EC50 of around 1 microM and XE991 was almost 10-fold more potent. Neither removal of the endothelium nor exposure to phentolamine or alpha,beta-methylene ATP, to block alpha1-adrenoceptors or P2X receptors, respectively, affected the contraction. Contraction was abolished in Ca2+-free solution and in the presence of 1 microM nifedipine or 10 microM levcromakalim.
The KCNQ channel blockers are potent and powerful constrictors of pulmonary arteries. This action may be selective for the pulmonary circulation as mesenteric arteries showed little response. The results imply that the drugs act directly on smooth muscle cells and contraction requires voltage-dependent Ca2+ influx. It is concluded that the drugs probably act by blocking KCNQ channels in pulmonary artery myocytes, leading to membrane depolarization and Ca2+ influx through L-type Ca2+ channels. This implies a functional role for KCNQ channels in regulating the resting membrane potential of pulmonary artery myocytes.
KCNQ通道已在神经系统、心脏和内耳中得到广泛研究,它们在这些部位具有重要的生理功能。最近的报道表明,KCNQ通道也可能在门静脉中表达,据推测它们会影响自发收缩活动。由KCNQ通道介导的钾电流的生物物理特性类似于肺动脉平滑肌细胞静息钾电导和静息电位所对应的电流。因此,我们通过测定选择性KCNQ通道阻滞剂利诺吡啶和XE991促进肺血管收缩的能力,来研究KCNQ通道在调节肺动脉功能中的可能作用。
使用小血管肌动描记法测量大鼠和小鼠肺内动脉或肠系膜动脉产生的张力。在完整血管和去内皮血管中测量对利诺吡啶和XE991的收缩反应。还在防止神经释放的去甲肾上腺素或ATP的收缩作用或阻断各种钙内流途径的条件下进行实验,以研究收缩的潜在机制。
利诺吡啶和XE991均可使大鼠和小鼠肺动脉收缩,但对肠系膜动脉影响很小。在每种情况下,最大收缩幅度几乎与对50 mM钾的反应一样大。利诺吡啶的半数有效浓度(EC50)约为1 microM,而XE991的效力几乎强10倍。去除内皮或分别暴露于酚妥拉明或α,β-亚甲基ATP以阻断α1-肾上腺素能受体或P2X受体,均不影响收缩。在无钙溶液以及存在1 microM硝苯地平或10 microM 左旋克罗卡林的情况下,收缩被消除。
KCNQ通道阻滞剂是肺动脉强效且有力的收缩剂。这种作用可能对肺循环具有选择性,因为肠系膜动脉几乎没有反应。结果表明,这些药物直接作用于平滑肌细胞,收缩需要电压依赖性钙内流。得出的结论是,这些药物可能通过阻断肺动脉肌细胞中的KCNQ通道起作用,导致膜去极化并通过L型钙通道使钙内流。这意味着KCNQ通道在调节肺动脉肌细胞静息膜电位方面具有功能作用。
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