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β-银环蛇毒素B亚基对钾通道的阻断作用。

Potassium channel blockade by the B subunit of beta-bungarotoxin.

作者信息

Benishin C G

机构信息

Department of Physiology, Faculty of Medicine, University of Alberta, Edmonton, Canada.

出版信息

Mol Pharmacol. 1990 Aug;38(2):164-9.

PMID:2385229
Abstract

beta-Bungarotoxin (beta-BTX) isolated from the venom of Bungarus multicinctus has previously been reported to be a neurotoxic protein. The toxin is composed of two subunit chains, denoted A and B. The intact toxin was first examined in this study for its ability to block central nerve ending K channels using the 86Rb efflux technique. beta-BTX, when preincubated with synaptosomes for 30 min in the absence of extracellular Ca2+, selectively inhibited the slowly inactivating voltage-dependent (S) component of 86Rb efflux. The EC50 for inhibition is 1 to 3 nM. The two subunit chains were separated and isolated by reduction and carboxymethylation of the parent toxin. The K channel-blocking activity was associated only with the reduced and carboxymethylated B-subunit of beta-BTX (RCM-B). The dose-dependent inhibition by RCM-B exhibited an apparent biphasic response, with the noninactivating voltage-gated K channel being more susceptible to RCM-B inhibition (EC50 = 0.1 to 0.3 nM) than to inhibition by the parent compound. Additionally, the inactivating voltage-gated K channel (T) was sensitive to inhibition by higher concentrations of RCM-B (EC50 = 1 to 3 nM). These results suggest that the B-chain of beta-BTX may be responsible for blockade of certain voltage-gated K channels in a manner that is not directly related to the known phospholipase activity of the intact molecule.

摘要

从多环眼镜蛇毒液中分离出的β-银环蛇毒素(β-BTX)此前被报道为一种神经毒性蛋白。该毒素由两条亚基链组成,分别称为A链和B链。在本研究中,首次使用86Rb外流技术检测了完整毒素阻断中枢神经末梢钾通道的能力。在无细胞外Ca2+的情况下,β-BTX与突触体预孵育30分钟后,选择性抑制了86Rb外流的缓慢失活电压依赖性(S)成分。抑制作用的半数有效浓度(EC50)为1至3 nM。通过对母毒素进行还原和羧甲基化,分离出了两条亚基链。钾通道阻断活性仅与β-BTX的还原羧甲基化B亚基(RCM-B)有关。RCM-B的剂量依赖性抑制表现出明显的双相反应,非失活电压门控钾通道比母化合物更易受到RCM-B的抑制(EC50 = 0.1至0.3 nM)。此外,失活电压门控钾通道(T)对较高浓度的RCM-B抑制敏感(EC50 = 1至3 nM)。这些结果表明,β-BTX的B链可能以一种与完整分子已知磷脂酶活性不直接相关的方式负责阻断某些电压门控钾通道。

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