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从伊朗蝎子毒液中纯化并鉴定一种作为药物工具的哺乳动物神经毒素及其分子特性

Purification and Molecular Characterization of a Mammalian Neurotoxin as a Pharmaceutical Tool from the Venom of Iranian Scorpion .

作者信息

Rabiei Hadi, Zare-Mirakabadi Abbas, Mohtat Bita, Mirza Behrooz

机构信息

Department of Chemistry, Karaj Branch, Islamic Azad University, Karaj, Iran.

Venomous Animals and Antivenom Production Department, Razi Vaccine and Serum Research Institute, Agricultural Research-Education and Extension Organization, Karaj, Iran.

出版信息

J Arthropod Borne Dis. 2024 Sep 30;18(3):238-252. doi: 10.18502/jad.v18i3.18575. eCollection 2024 Sep.

Abstract

BACKGROUND

Venom of scorpions are complex bioactive polypeptides. To gain greater insights into the structural and functional impacts of toxins from (Buthidae) a dangerously venomous scorpion species, its venom was isolated, purified, and characterized.

METHODS

Long chain toxin with four disulfide bonds purified by size exclusion chromatography and reversed-phase HPLC and characterized by amino acid sequencing and molecular weight determination.

RESULTS

The primary structure analysis exhibits a neurotoxin named AnCra2 with 7302.24 Da molecular weight and 64 amino acid residues that cause paralysis and lead to death in NIH mice. The LD of AnCra2 was determined to be 0.61±0.04 μg/mice. Phylogenetic analysis displays the toxin has 97% sequence similarity with alpha toxins reported from north African scorpions that affect voltage-gated sodium channels (VGSC), also proposed that differentiation among the scorpions of family Buthidae is affected by the geographical conditions and efficiency in evolutionary variations. AnCra2 exposed binding residues have a high affinity for receptor residues in site-3 (segment-3) of VGSC that are approved by three-dimensional structure and homology modeling.

CONCLUSION

Purified AnCra2 seems to be a new putative Alpha neurotoxin in homology with the structure of neurotoxins that act on VGSC as a pharmaceutical tool.

摘要

背景

蝎子毒液是复杂的生物活性多肽。为了更深入了解一种危险的有毒蝎子物种(钳蝎科)毒素的结构和功能影响,对其毒液进行了分离、纯化和表征。

方法

通过尺寸排阻色谱和反相高效液相色谱法纯化具有四个二硫键的长链毒素,并通过氨基酸测序和分子量测定进行表征。

结果

一级结构分析显示一种名为AnCra2的神经毒素,分子量为7302.24 Da,有64个氨基酸残基,可导致NIH小鼠麻痹并致死。AnCra2的半数致死量测定为0.61±0.04 μg/小鼠。系统发育分析表明,该毒素与北非蝎子报道的影响电压门控钠通道(VGSC)的α毒素有97%的序列相似性,也表明钳蝎科蝎子之间的分化受地理条件和进化变异效率的影响。AnCra2暴露的结合残基对VGSC第3位点(第3片段)的受体残基具有高亲和力,这通过三维结构和同源建模得到证实。

结论

纯化的AnCra2似乎是一种新的假定α神经毒素,与作用于VGSC的神经毒素结构同源,可作为一种药物工具。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/48d9/12144856/1baa03a72c6f/JAD-18-238-g001.jpg

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