哺乳动物红细胞中钙激活钾通透性某些阻滞剂作用的差异。

Differences in the actions of some blockers of the calcium-activated potassium permeability in mammalian red cells.

作者信息

Benton D C, Roxburgh C J, Ganellin C R, Shiner M A, Jenkinson D H

机构信息

Department of Pharmacology, University College London.

出版信息

Br J Pharmacol. 1999 Jan;126(1):169-78. doi: 10.1038/sj.bjp.0702292.

DOI:10.1038/sj.bjp.0702292

PMID:10051133

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1565796/

Abstract

The actions of some inhibitors of the Ca2+-activated K+ permeability in mammalian red cells have been compared. 2. Block of the permeability was assessed from the reduction in the net loss of K+ that followed the application of the Ca2+ ionophore A23187 (2 microM) to rabbit red cells suspended at a haematocrit of 1% in a low potassium solution ([K]0 0.12-0.17 mM) at 37 degrees C. Net movement of K+ was measured using a K+-sensitive electrode placed in the suspension. 3. The concentrations (microM +/- s.d.) of the compounds tested causing 50% inhibition of K+ loss were: quinine, 37 +/- 3; cetiedil, 26 +/- 1; the cetiedil congeners UCL 1269, UCL 1274 and UCL 1495, approximately 150, 8.2 +/- 0.1, 0.92 +/- 0.03 respectively; clotrimazole, 1.2 +/- 0.1; nitrendipine, 3.6 +/- 0.5 and charybdotoxin, 0.015 +/- 0.002. 4. The characteristics of the block suggested that compounds could be placed in two groups. For one set (quinine, cetiedil, and the UCL congeners), the concentration-inhibition curves were steeper (Hill coefficient, nH, > or = 2.7) than for the other (clotrimazole, nitrendipine, charybdotoxin) for which nH approximately 1. 5. Compounds in the first set alone became less active on raising the concentration of K+ in the external solution to 5.4 mM. 6. The rate of K+ loss induced by A23187 slowed in the presence of high concentrations of cetiedil and its analogues, suggesting a use-dependent component to the inhibitory action. This was not seen with clotrimazole. 7. The blocking action of the cetiedil analogue UCL 1274 could not be overcome by an increase in external Ca2+ and its potency was unaltered when K+ loss was induced by the application of Pb2+ (10 microM) rather than by A23187. 8. These results, taken with the findings of others, suggest that agents that block the red cell Ca2+-activated K+ permeability can be placed in two groups with different mechanisms of action. The differences can be explained by supposing that clotrimazole and charybdotoxin act at the outer face of the channel whereas cetiedil and its congeners may block within it, either at or near the K+ binding site that determines the flow of K+.

摘要

对哺乳动物红细胞中一些钙激活钾通透性抑制剂的作用进行了比较。2. 通过将钙离子载体A23187（2微摩尔）应用于悬浮在37℃下低钾溶液（[K]0 0.12 - 0.17毫摩尔）中、血细胞比容为1%的兔红细胞后，钾净损失的减少来评估通透性的阻断情况。使用置于悬浮液中的钾敏感电极测量钾的净移动。3. 导致50%钾损失抑制的受试化合物浓度（微摩尔±标准差）为：奎宁，37±3；西替地尔，26±1；西替地尔同系物UCL 1269、UCL 1274和UCL 1495，分别约为150、8.2±0.1、0.92±0.03；克霉唑，1.2±0.1；尼群地平，3.6±0.5；蝎毒素，0.015±0.002。4. 阻断特性表明化合物可分为两组。对于一组（奎宁、西替地尔和UCL同系物），浓度 - 抑制曲线比另一组（克霉唑、尼群地平、蝎毒素）更陡（希尔系数，nH，≥2.7），后者nH约为1。5. 仅第一组中的化合物在将外部溶液中钾浓度提高到5.4毫摩尔时活性降低。6. 在高浓度西替地尔及其类似物存在下，A23187诱导的钾损失速率减慢，表明抑制作用存在使用依赖性成分。克霉唑未观察到这种情况。7. 西替地尔类似物UCL 1274的阻断作用不能通过增加外部钙来克服，并且当通过应用Pb2 +（10微摩尔）而非A23187诱导钾损失时，其效力不变。8. 这些结果与其他人的发现一起表明，阻断红细胞钙激活钾通透性的药物可分为两组，作用机制不同。这些差异可以通过假设克霉唑和蝎毒素作用于通道外表面，而西替地尔及其同系物可能在通道内阻断，要么在决定钾流动的钾结合位点处，要么在其附近来解释。