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东亚钳蝎毒液中的两种神经毒素(BmK I和BmK II):纯化、氨基酸序列及比活性评估。

Two neurotoxins (BmK I and BmK II) from the venom of the scorpion Buthus martensi Karsch: purification, amino acid sequences and assessment of specific activity.

作者信息

Ji Y H, Mansuelle P, Terakawa S, Kopeyan C, Yanaihara N, Hsu K, Rochat H

机构信息

Shanghai Institute of Physiology, Chinese Academy of Sciences, P.R. China.

出版信息

Toxicon. 1996 Sep;34(9):987-1001. doi: 10.1016/0041-0101(96)00065-7.

Abstract

Two neurotoxins, BmK I and BmK II, were purified from the venom of the Chinese scorpion Buthus martensi Karsch. The complete amino acid sequences of both toxins, each containing 64 amino acid residues, were determined by the automatic sequencing of reduced and S-carboxymethylated toxins and their peptides, obtained after cleavage with TPCK-treated trypsin and Staphylococcus aureus V8 protease, respectively. Toxicity as minimum lethal dose tested by i.c.v. injection in mice showed that BmK I was six times more potent than BmK II. Only two amino acid replacements were found: at position 59 Val in BmK I was replaced by Ile in BmK II, and at position 62 a basic Lys residue in BmK I was substituted by a neutral Asn residue in BmK II. These features suggest that the positively charged residue (Lys or Arg) in the C-terminal position 62 (or 61 or 63) may also play an important role in facilitating the interaction between scorpion neurotoxins and the receptor on sodium channels. The effects of BmK I on nerve excitability were examined with the crayfish axon using intracellular recording and voltage-clamp conditions. The results indicate that BmK I preferentially blocks the sodium channel inactivation process. Thus, functional and structural similarities suggest that BmK I and BmK II belong to group 3 of scorpion alpha-type toxins.

摘要

从中国蝎子东亚钳蝎(Buthus martensi Karsch)的毒液中纯化出了两种神经毒素,即BmK I和BmK II。这两种毒素的完整氨基酸序列均包含64个氨基酸残基,分别通过对还原型和S-羧甲基化毒素及其肽段进行自动测序来确定,这些肽段是在用经TPCK处理的胰蛋白酶和金黄色葡萄球菌V8蛋白酶分别切割后获得的。通过小鼠脑室内注射测定的最小致死剂量毒性表明,BmK I的毒性比BmK II强六倍。仅发现两个氨基酸替换:在第59位,BmK I中的缬氨酸被BmK II中的异亮氨酸取代;在第62位,BmK I中的碱性赖氨酸残基被BmK II中的中性天冬酰胺残基取代。这些特征表明,C末端第62位(或61位或63位)的带正电荷残基(赖氨酸或精氨酸)在促进蝎子神经毒素与钠通道上的受体之间的相互作用中可能也起着重要作用。使用细胞内记录和电压钳制条件,在小龙虾轴突上研究了BmK I对神经兴奋性的影响。结果表明,BmK I优先阻断钠通道失活过程。因此,功能和结构上的相似性表明,BmK I和BmK II属于蝎子α型毒素的第3组。

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