Sahinturk Serdar, Demirel Sadettin, Ozyener Fadil, Isbil Naciye
Physiology Department, Bursa Uludag University Medicine School, Bursa, Turkey.
Gen Physiol Biophys. 2021 Sep;40(5):427-434. doi: 10.4149/gpb_20210258.
In this study, the effect and effect mechanisms of [Pyr1]apelin-13, the dominant apelin isoform in the human cardiovascular tissues and human plasma, on vascular contractility were investigated. The vascular rings obtained from the thoracic aortas of the male Wistar Albino rats were placed in the isolated tissue bath system. After the equilibration period, [Pyr1]apelin-13 (10-9 to 10-6 M) was applied cumulatively to the aortic rings pre-contracted with phenylephrine in the plateau phase. The protocol was repeated in the presence of specific signaling pathway inhibitors (F13A, L-NAME, dorsomorphin, TEA, U0126, or indomethacin) to determine the effect mechanisms of [Pyr1]apelin-13. [Pyr1]apelin-13 induced a dose-dependent relaxation in the pre-contracted aortic rings. APJ, eNOS, AMPK, and potassium channel inhibition statistically significantly decreased the vasodilator effect of [Pyr1]apelin-13. MAPK and COX inhibition didn't statistically significantly changed the vasodilator effect of [Pyr1]apelin-13. In conclusion, [Pyr1]apelin-13 relaxes the rat thoracic aorta via APJ, NO, AMPK, and potassium channels.
在本研究中,对人体心血管组织和人体血浆中主要的apelin亚型[Pyr1]apelin-13对血管收缩性的作用及其作用机制进行了研究。从雄性Wistar白化大鼠的胸主动脉获取血管环,并将其置于离体组织浴系统中。在平衡期后,将[Pyr1]apelin-13(10-9至10-6 M)累积应用于处于平台期且已用去氧肾上腺素预收缩的主动脉环。在存在特定信号通路抑制剂(F13A、L-NAME、多司莫德、TEA、U0126或吲哚美辛)的情况下重复该实验方案,以确定[Pyr1]apelin-13的作用机制。[Pyr1]apelin-13在预收缩的主动脉环中诱导剂量依赖性舒张。APJ、eNOS、AMPK和钾通道抑制在统计学上显著降低了[Pyr1]apelin-13的血管舒张作用。MAPK和COX抑制在统计学上未显著改变[Pyr1]apelin-13的血管舒张作用。总之,[Pyr1]apelin-13通过APJ、NO、AMPK和钾通道使大鼠胸主动脉舒张。
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