蝎毒素在体外与钠通道的结合及其被β-银环蛇毒素的修饰

Binding of scorpion toxin to sodium channels in vitro and its modification by beta-bungarotoxin.

作者信息

Okamoto H

出版信息

J Physiol. 1980 Feb;299:507-20. doi: 10.1113/jphysiol.1980.sp013139.

DOI:10.1113/jphysiol.1980.sp013139

PMID:6247482

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1279239/

Abstract

Binding of a purified scorpion toxin to membrane fragments isolated from electroplaque of an electric eel Electrophorus electricus was studied using a radio-iodinated toxin.2. A scorpion toxin was purified from the venom of Leiurus quinquestriatus and iodinated with (125)I in a lactoperoxidase-catalysed reaction. Monoiodinated toxin, isolated by an ion exchange chromatography, retarded the inactivation kinetics of Na current to a similar extent as the native toxin, indicating that radioiodination did not appreciably affect physiological and binding properties of the native toxin.3. Analyses of binding properties by Scatchard plots showed the presence of two classes of binding sites (with low and high affinities) in the membrane preparation from eel electroplaque; similar preparation from an electric skate, of which the electroplaque is known to be devoid of Na channels, possessed only the low affinity sites.4. The number of high affinity sites in the eel preparation was 41.8 +/- 10.5 p-mole/g tissue; the value was within the range reported for tetrodotoxin binding to similar preparations (15-148 p-mole/g tissue).5. A variety of cations (Na(+), Mn(2+) and La(3+)) inhibited the high affinity scorpion toxin binding, as indicated for the toxin binding to Na channels by a previous electrophysiological study. K(D) value in the presence of 120 mM-Na(+) (approx. 8 nM) agreed reasonably with that (approx. 10nM) reported for the scorpion toxin binding to excitable neuroblastoma cells or synaptic nerve ending particles under conditions where membrane potential was depolarized by the addition of 135 mM-KCl.6. Pretreatment of the eel membrane preparation with beta-bungarotoxin (7-44 ng/ml.) in the presence of Ca ions (10-200 muM) resulted in a substantial loss of high affinity binding of scorpion toxin. When phospholipase A(2) activity of the beta-toxin was inactivated by a chemical modification with p-bromophenacyl bromide, the inhibitory action of the beta-bungarotoxin was abolished.7. It is concluded that a high affinity binding of scorpion toxin to the eel electroplaque membrane fragments represents the binding to Na channels in vitro, and that phospholipase A(2) activity of beta-bungarotoxin interferes with the binding of scorpion toxin to Na channels.

摘要

使用放射性碘化毒素研究了一种纯化的蝎毒素与从电鳗（电鳐）电板分离的膜片段的结合情况。
从金蝎毒液中纯化出一种蝎毒素，并在乳过氧化物酶催化反应中用（125）I进行碘化。通过离子交换色谱分离得到的单碘化毒素，使钠电流的失活动力学延迟的程度与天然毒素相似，这表明放射性碘化并未明显影响天然毒素的生理和结合特性。
通过Scatchard图分析结合特性表明，在电鳗电板的膜制剂中存在两类结合位点（低亲和力和高亲和力）；而电鳐的类似制剂（已知其电板不含钠通道）仅具有低亲和力位点。
电鳗制剂中高亲和力位点的数量为41.8±10.5皮摩尔/克组织；该值在报道的河豚毒素与类似制剂结合的范围内（15 - 148皮摩尔/克组织）。
多种阳离子（Na⁺、Mn²⁺和La³⁺）抑制高亲和力蝎毒素结合，如先前的电生理研究表明毒素与钠通道的结合情况。在120 mM - Na⁺存在下的K（D）值（约8 nM）与报道的在通过添加135 mM - KCl使膜电位去极化的条件下蝎毒素与可兴奋神经母细胞瘤细胞或突触神经末梢颗粒结合的K（D）值（约10 nM）相当吻合。
在钙离子（10 - 200 μM）存在下，用β - 银环蛇毒素（7 - 44 ng/ml）预处理电鳗膜制剂，导致蝎毒素高亲和力结合大量丧失。当用对溴苯甲酰溴进行化学修饰使β - 毒素的磷脂酶A₂活性失活时，β - 银环蛇毒素的抑制作用被消除。
得出结论：蝎毒素与电鳗电板膜片段的高亲和力结合代表了体外与钠通道的结合，并且β - 银环蛇毒素的磷脂酶A₂活性干扰了蝎毒素与钠通道的结合。