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钙调蛋白参与小鼠成纤维细胞中钙激活钾通道运作的证据。

Evidence for the involvement of calmodulin in the operation of Ca-activated K channels in mouse fibroblasts.

作者信息

Okada Y, Yada T, Ohno-Shosaku T, Oiki S

出版信息

J Membr Biol. 1987;96(2):121-8. doi: 10.1007/BF01869238.

Abstract

The oscillation of membrane potential in fibroblastic L cells is known to result from periodic stimulation of Ca2+-activated K+ channels due to the oscillatory increase in the intracellular Ca2+ concentration. These repeated hyperpolarizations were inhibited by putative calmodulin antagonists, trifluoperazine (TFP), N-(6-aminohexyl)-5-chloro-1-naphthalenesulfonamide (W-7) and promethazine (PMZ), and the concentrations required for half-maximal inhibition were 25, 30 and 300 microM, respectively. These doses were lower than those for reducing the membrane resistance due to nonspecific cell damages. Another calmodulin antagonist, chlorpromazine (CPZ), was also effective, but CPZ-sulfoxide was not. Intracellular pressure injections of calmodulin-interacting divalent cations, Ca2+, Sr2+, Mn2+ and Ni2+, elicited slow hyperpolarizations, whereas Mg2+ and Ba2+, which are known to be essentially inert for calmodulin, failed to evoke any responses. The injection of purified calmodulin also brought about a similar hyperpolarization. Quinine, an inhibitor of Ca2+-activated K+ channels, abolished both Ca2+- and calmodulin-induced hyperpolarizations. TFP prevented Ca2+-induced hyperpolarizations. The TFP effect was partially reversed by the calmodulin injection. It is concluded that calmodulin is involved in the operation of Ca2+-activated K+ channels in fibroblasts.

摘要

已知成纤维细胞L细胞膜电位的振荡是由于细胞内Ca2+浓度的振荡增加对Ca2+激活的K+通道进行周期性刺激所致。这些反复出现的超极化被公认的钙调蛋白拮抗剂三氟拉嗪(TFP)、N-(6-氨基己基)-5-氯-1-萘磺酰胺(W-7)和异丙嗪(PMZ)所抑制,半最大抑制所需浓度分别为25、30和300微摩尔。这些剂量低于因非特异性细胞损伤而降低膜电阻所需的剂量。另一种钙调蛋白拮抗剂氯丙嗪(CPZ)也有效,但氯丙嗪亚砜无效。向细胞内压力注射与钙调蛋白相互作用的二价阳离子Ca2+、Sr2+、Mn2+和Ni2+可引起缓慢的超极化,而众所周知对钙调蛋白基本无活性的Mg2+和Ba2+未能引发任何反应。注射纯化的钙调蛋白也会引起类似的超极化。Ca2+激活的K+通道抑制剂奎宁消除了Ca2+和钙调蛋白诱导的超极化。TFP阻止了Ca2+诱导的超极化。钙调蛋白注射可部分逆转TFP的作用。结论是钙调蛋白参与了成纤维细胞中Ca2+激活的K+通道的运作。

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