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蛇毒突触前毒素的磷脂酶A2活性及底物特异性

Phospholipase A2 activity and substrate specificity of snake venom presynaptic toxins.

作者信息

Napias C, Heilbronn E

出版信息

Biochemistry. 1980 Mar 18;19(6):1146-51. doi: 10.1021/bi00547a017.

Abstract

Beta-Neurotoxins from certain snake venoms are highly specific toxins acting at the presynaptic side of the neuromuscular junction. In this study biochemical aspects of this high specificity have been investigated. When toxins (notexin and Naja nigricollis basic phospholipase) act on a mixture of subcellular fractions obtained from brain cortex (synaptosomes, myelin, and mitochondria), the synaptosomal fraction is preferentially attacked and shows the highest release of membrane protein. As seen from isolated fractions, however, even the mitochondria are rapidly and strongly attached. Examining the phospholipase A2 activity of the toxin instead of the release of proteins reveals that synaptosomes represent the best substrate. In contrast to nonneurotoxic phospholipases A2, that from neurotoxin preferentially uses synaptosomal phosphatidylcholine as a substrate when pure phospholipids isolated from subcellular fractions are used. A relationship between the cholesterol/phospholipid ratio and the sensitivity to toxin action in the various subcellular fractions was found. These data suggest that the neurotoxic effect is mainly due to the substrate specificity of the beta-neurotoxins. It is suggested that synaptosomal phosphatidylcholine, embedded in a membrane containing a low amount of cholesterol, is a highly specific substrate for beta-neurotoxins.

摘要

某些蛇毒中的β-神经毒素是作用于神经肌肉接头突触前侧的高度特异性毒素。在本研究中,对这种高度特异性的生化方面进行了研究。当毒素(诺维毒素和黑颈眼镜蛇碱性磷脂酶)作用于从大脑皮层获得的亚细胞组分混合物(突触体、髓磷脂和线粒体)时,突触体组分受到优先攻击,并显示出最高的膜蛋白释放量。然而,从分离的组分来看,即使是线粒体也会迅速且强烈地附着。检测毒素的磷脂酶A2活性而非蛋白质释放量发现,突触体是最佳底物。与非神经毒性磷脂酶A2不同,当使用从亚细胞组分中分离出的纯磷脂时,神经毒素来源的磷脂酶A2优先将突触体磷脂酰胆碱用作底物。发现了胆固醇/磷脂比率与各种亚细胞组分中对毒素作用的敏感性之间的关系。这些数据表明,神经毒性作用主要归因于β-神经毒素的底物特异性。有人提出,嵌入含少量胆固醇膜中的突触体磷脂酰胆碱是β-神经毒素的高度特异性底物。

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