在2至3月龄大鼠中,大电导钙激活钾通道会显著抑制动脉Kv7通道的功能可用性,但在10至15日龄大鼠中则不会。
The Functional Availability of Arterial Kv7 Channels Is Suppressed Considerably by Large-Conductance Calcium-Activated Potassium Channels in 2- to 3-Month Old but Not in 10- to 15-Day Old Rats.
作者信息
Ma Dongyu, Gaynullina Dina, Schmidt Nadine, Mladenov Mitko, Schubert Rudolf
机构信息
European Center for Angioscience (ECAS), Research Division Cardiovascular Physiology, Medical Faculty Mannheim, Heidelberg University, Mannheim, Germany.
Department of Cardiology, The First Affiliated Hospital of Anhui Medical University, Anhui, China.
出版信息
Front Physiol. 2020 Dec 15;11:597395. doi: 10.3389/fphys.2020.597395. eCollection 2020.
BACKGROUND
Voltage-gated potassium (Kv) channels, especially Kv7 channels, are major potassium channels identified in vascular smooth muscle cells with a great, albeit differential functional impact in various vessels. Vascular smooth muscle Kv7 channels always coexist with other K channels, in particular with BK channels. BK channels differ in the extent to which they influence vascular contractility. Whether this difference also causes the variability in the functional impact of Kv7 channels is unknown. Therefore, this study addressed the hypothesis that the functional impact of Kv7 channels depends on BK channels.
EXPERIMENTAL APPROACH
Experiments were performed on young and adult rat and arteries using real-time PCR as well as pressure and wire myography.
KEY RESULTS
Several subfamily members of Kv7 (KCNQ) and BK channels were expressed in saphenous and gracilis arteries: the highest expression was observed for BKα, BKβ1 and KCNQ4. Arterial contractility was assessed with methoxamine-induced contractions and pressure-induced myogenic responses. In vessels of adult rats, inhibition of Kv7 channels or BK channels by XE991 or IBTX, respectively enhanced arterial contractility to a similar degree, whereas activation of Kv7 channels or BK channels by retigabine or NS19504, respectively reduced arterial contractility to a similar degree. Further, IBTX increased both the contractile effect of XE991 and the anticontractile effect of retigabine, whereas NS19504 reduced the effect of retigabine and impaired the effect of XE991. In vessels of young rats, inhibition of Kv7 channels by XE991 enhanced arterial contractility much stronger than inhibition of BK channels by IBTX, whereas activation of Kv7 by retigabine reduced arterial contractility to a greater extent than activation of BK channels by NS19504. Further, IBTX increased the anticontractile effect of retigabine but not the contractile effect of XE991, whereas NS19504 reduced the effect of retigabine and impaired the effect of XE991.
CONCLUSION
Kv7 and BK channels are expressed in young and adult rat arteries and function as negative feedback modulators in the regulation of contractility of these arteries. Importantly, BK channels govern the extent of functional impact of Kv7 channels. This effect depends on the relationship between the functional activities of BK and Kv7 channels.
背景
电压门控钾(Kv)通道,尤其是Kv7通道,是在血管平滑肌细胞中发现的主要钾通道,尽管在不同血管中其功能影响存在差异。血管平滑肌Kv7通道总是与其他钾通道共存,特别是与大电导钙激活钾(BK)通道。BK通道对血管收缩性的影响程度各不相同。这种差异是否也导致了Kv7通道功能影响的变异性尚不清楚。因此,本研究探讨了Kv7通道的功能影响取决于BK通道这一假说。
实验方法
使用实时定量聚合酶链反应(real-time PCR)以及压力和线张力肌描记法对幼年和成年大鼠的隐动脉和股薄肌动脉进行实验。
关键结果
Kv7(KCNQ)和BK通道的几个亚家族成员在隐动脉和股薄肌动脉中表达:BKα、BKβ1和KCNQ4的表达最高。用甲氧明诱导的收缩和压力诱导的肌源性反应评估动脉收缩性。在成年大鼠的血管中,分别用XE991或IBTX抑制Kv7通道或BK通道,动脉收缩性增强程度相似,而分别用瑞替加滨或NS19504激活Kv7通道或BK通道,动脉收缩性降低程度相似。此外,IBTX增加了XE991的收缩作用和瑞替加滨的抗收缩作用,而NS19504降低了瑞替加滨的作用并削弱了XE991的作用。在幼年大鼠的血管中,XE991抑制Kv7通道比IBTX抑制BK通道增强动脉收缩性的作用更强,而瑞替加滨激活Kv7通道比NS19504激活BK通道降低动脉收缩性的程度更大。此外,IBTX增加了瑞替加滨的抗收缩作用,但未增加XE991的收缩作用,而NS19504降低了瑞替加滨的作用并削弱了XE991的作用。
结论
Kv7和BK通道在幼年和成年大鼠动脉中表达,并在这些动脉收缩性调节中作为负反馈调节因子发挥作用。重要的是,BK通道决定了Kv7通道功能影响的程度。这种效应取决于BK和Kv7通道功能活动之间的关系。
Zotero 插件