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细胞色素P450抑制剂对大鼠门静脉钾电流和机械活性的影响。

Effects of cytochrome P450 inhibitors on potassium currents and mechanical activity in rat portal vein.

作者信息

Edwards G, Zygmunt P M, Högestätt E D, Weston A H

机构信息

School of Biological Sciences, University of Manchester.

出版信息

Br J Pharmacol. 1996 Oct;119(4):691-701. doi: 10.1111/j.1476-5381.1996.tb15728.x.

DOI:10.1111/j.1476-5381.1996.tb15728.x
PMID:8904643
原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1915770/
Abstract
  1. The effects of the cytochrome P450 inhibitors, proadifen, clotrimazole and 17-octadecynoic acid (17-ODYA) on K-currents in freshly-isolated single cells derived from rat portal vein and on mechanical activity in whole veins were studied. 2. When cells were stepped from -90 mV to a series of test potentials (from -80 to +50 mV), a delayed rectifier current (IK(V)) and an A-type current (IK(A)) could be identified. Proadifen (10 microM), clotrimazole (30 microM) and 17-ODYA (5 microM) each inhibited IK(V) but had little effect on IK(A). 3. When cells were held at -10 mV to inactivate the time-dependent K-currents, IK(V) and IK(A), levcromakalim (3 microM) induced a time-independent outward K-current (IK(ATP)) which was totally inhibited by clotrimazole (30 microM) and almost fully inhibited by proadifen (10 microM). 17-ODYA (5 microM) had no effect on IK(ATP) and exerted only a minor inhibitory action on this current at 20 microM. 4. 17-ODYA (5 microM) potentiated current flow through the large conductance, Ca-sensitive K-channel (BKCa). In contrast, proadifen (10 microM) had no effect on IBK(Ca) whereas clotrimazole (30 microM) exerted a small but significant inhibitory action. 5. Proadifen (10 microM) and clotrimazole (30 microM) each inhibited the magnitude but increased the frequency of spontaneous contractions in whole portal veins. 17-ODYA (5 microM) had no effect on spontaneous contractions but these were inhibited when the concentration of 17-ODYA was increased to 50 microM. 6. The spasmolytic effect of levcromakalim on spontaneous contractions was antagonized by proadifen (10-30 microM) in a concentration-dependent manner but 17-ODYA (up to 50 microM) was without effect. 7. These results in portal vein show that cytochrome P450 inhibitors exert profound effects on a variety of K-channel subtypes. This suggests that enzymes dependent on this cofactor may be important regulators of K-channel activity in smooth muscle. The relevance of these findings for the identification of the pathway involved in the synthesis of the endothelium-derived hyperpolarizing factor is discussed.
摘要
  1. 研究了细胞色素P450抑制剂丙胺太林、克霉唑和17-十八碳炔酸(17-ODYA)对大鼠门静脉新鲜分离的单细胞钾电流以及对整个静脉机械活性的影响。2. 当细胞从-90 mV跃迁至一系列测试电位(从-80至+50 mV)时,可识别出延迟整流电流(IK(V))和A型电流(IK(A))。丙胺太林(10 microM)、克霉唑(30 microM)和17-ODYA(5 microM)均抑制IK(V),但对IK(A)影响较小。3. 当细胞保持在-10 mV以使时间依赖性钾电流IK(V)和IK(A)失活时,左旋克罗卡林(3 microM)诱导出一种时间非依赖性外向钾电流(IK(ATP)),该电流被克霉唑(30 microM)完全抑制,被丙胺太林(10 microM)几乎完全抑制。17-ODYA(5 microM)对IK(ATP)无影响,在20 microM时对该电流仅产生轻微抑制作用。4. 17-ODYA(5 microM)增强了通过大电导钙敏感钾通道(BKCa)的电流。相比之下,丙胺太林(10 microM)对IBK(Ca)无影响,而克霉唑(30 microM)则产生小但显著的抑制作用。5. 丙胺太林(10 microM)和克霉唑(30 microM)均抑制整个门静脉自发收缩的幅度,但增加其频率。17-ODYA(5 microM)对自发收缩无影响,但当17-ODYA浓度增加至50 microM时则抑制自发收缩。6. 左旋克罗卡林对自发收缩的解痉作用被丙胺太林(10 - 30 microM)以浓度依赖性方式拮抗,但17-ODYA(高达50 microM)无作用。7. 门静脉的这些结果表明,细胞色素P450抑制剂对多种钾通道亚型有深远影响。这表明依赖该辅因子的酶可能是平滑肌中钾通道活性的重要调节因子。讨论了这些发现对于确定内皮源性超极化因子合成所涉及途径的相关性。

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