一氧化氮通过激活大电导钙激活钾通道介导血管紧张素原诱导的大鼠离体冠状动脉舒张。
Activation of Large Conductance, Calcium-Activated Potassium Channels by Nitric Oxide Mediates Apelin-Induced Relaxation of Isolated Rat Coronary Arteries.
机构信息
Department of Pharmaceutical Sciences, North Dakota State University, Fargo, North Dakota.
Department of Pharmaceutical Sciences, North Dakota State University, Fargo, North Dakota
出版信息
J Pharmacol Exp Ther. 2018 Aug;366(2):265-273. doi: 10.1124/jpet.118.248682. Epub 2018 May 17.
Apelin increases coronary blood flow, cardiac contractility, and cardiac output. Based on these favorable hemodynamic effects, apelin and apelin-like analogs are being developed for treating heart failure and related disorders; however, the molecular mechanisms underlying apelin-induced coronary vasodilation are unknown. This study aimed to elucidate the signaling pathways by which apelin causes smooth muscle relaxation in coronary arteries. Receptors for apelin (APJ receptors) were expressed in coronary arteries, as determined by Western blot and polymerase chain reaction analyses. Immunofluorescence imaging studies identified APJ receptors on endothelial and smooth muscle cells. In isolated endothelial cells, apelin caused an increase in 4,5-diaminofluorescein fluorescence that was abolished by nitro-l-arginine (NLA) and F13A (H-Gln-Arg-Pro-Arg-Leu-Ser-His-Lys-Gly-Pro-Met-Pro-Ala-OH), an APJ receptor antagonist, consistent with increased nitric oxide (NO) production. In arterial rings, apelin caused endothelium-dependent relaxations that were abolished by NLA, F13A, and iberiotoxin. Neither oxadiazolo[4,3-]quinoxalin-1-one (ODQ) nor DT-2, a protein kinase G inhibitor, had any effect on apelin-induced relaxations, and apelin itself had no effect on intracellular cGMP accumulation in coronary arteries. Patch-clamp studies in isolated smooth muscle cells demonstrated that the NO donors, diethyl amine NONOate and sodium nitroprusside, caused increases in large conductance, calcium-activated potassium channel (BK) currents, which were inhibited by iberiotoxin but not ODQ. Thus, apelin causes endothelium-dependent relaxation of coronary arteries by stimulating endothelial APJ receptors and releasing NO, which acts in a cGMP-independent manner and increases BK activity in the underlying smooth muscle cells. These results provide a mechanistic basis for apelin-induced coronary vasodilation and may provide guidance for the future development of novel apelin-like therapeutic agents.
Apelin 增加冠状动脉血流量、心肌收缩力和心输出量。基于这些有利的血液动力学效应,apelin 和 apelin 类似物正在被开发用于治疗心力衰竭和相关疾病;然而,apelin 诱导冠状动脉扩张的分子机制尚不清楚。本研究旨在阐明 apelin 引起冠状动脉平滑肌松弛的信号通路。通过 Western blot 和聚合酶链反应分析确定了冠状动脉中 apelin 的受体 (APJ 受体)。免疫荧光成像研究确定了内皮细胞和平滑肌细胞上的 APJ 受体。在分离的内皮细胞中,apelin 引起 4,5-二氨基荧光素荧光的增加,该增加被硝基-L-精氨酸 (NLA) 和 F13A (H-Gln-Arg-Pro-Arg-Leu-Ser-His-Lys-Gly-Pro-Met-Pro-Ala-OH) 消除,后者是 APJ 受体拮抗剂,与一氧化氮 (NO) 产生增加一致。在动脉环中,apelin 引起内皮依赖性松弛,该松弛被 NLA、F13A 和 Iberiotoxin 消除。Oxadiazolo[4,3-]quinoxalin-1-one (ODQ) 和蛋白激酶 G 抑制剂 DT-2 均对 apelin 诱导的松弛没有影响,apelin 本身对冠状动脉中细胞内 cGMP 积累也没有影响。在分离的平滑肌细胞中的膜片钳研究表明,NO 供体二乙胺 NONOate 和硝普钠引起大电导、钙激活钾通道 (BK) 电流增加,该增加被 Iberiotoxin 抑制但不被 ODQ 抑制。因此,apelin 通过刺激内皮细胞 APJ 受体和释放一氧化氮来引起冠状动脉的内皮依赖性松弛,一氧化氮以 cGMP 非依赖性方式起作用并增加平滑肌细胞下的 BK 活性。这些结果为 apelin 诱导的冠状动脉扩张提供了机制基础,并可能为新型 apelin 样治疗剂的未来发展提供指导。
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