Recombinant expression and antigenicity of two peptide families of neurotoxins from Androctonus sp.

IF 1.8 3区医学 Q4 TOXICOLOGY

Journal of Venomous Animals and Toxins Including Tropical Diseases Pub Date : 2022-01-01 DOI:10.1590/1678-9199-JVATITD-2022-0026

Samuel Cardoso-Arenas, Herlinda Clement, Iván Arenas, Felipe Olvera, Fernando Zamudio, Figen Caliskan, Ligia Luz Corrales-García, Gerardo Corzo

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引用次数: 1

Abstract

Background: Scorpion neurotoxins such as those that modify the mammalian voltage-gated sodium ion channels (Nav) are the main responsible for scorpion envenomation. Their neutralization is crucial in the production of antivenoms against scorpion stings.

Methods: In the present study, two in silico designed genes - one that codes for a native neurotoxin from the venom of the Anatolian scorpion Androctonus crassicauda, named Acra 4 - and another non-native toxin - named consensus scorpion toxin (SccTx) obtained from the alignment of the primary structures of the most toxic neurotoxins from the Middle Eastern and North African scorpions - were recombinantly expressed in E. coli Origami.

Results: Following bacterial expression, the two expressed neurotoxins, hereafter named HisrAcra4 and HisrSccTx, were obtained from inclusion bodies. Both recombinant neurotoxins were obtained in multiple Cys-Cys isoforms. After refolding, the active protein fractions were identified with molecular masses of 8,947.6 and 9,989.1 Da for HisrAcra4 and HisrSccTx, respectively, which agreed with their expected theoretical masses. HisrAcra4 and HisrSccTx were used as antigens to immunize two groups of rabbits, to produce either anti-HisrAcra4 or anti-HisrSccTx serum antibodies, which in turn could recognize and neutralize neurotoxins from venoms of scorpion species from the Middle East and North Africa. The antibodies obtained from rabbits neutralized the 3LD₅₀ of Androctonus australis, Leiurus quinquestriatus hebraeus and Buthus occitanus venoms, but they did not neutralize A. crassicauda and A. mauritanicus venoms. In addition, the anti-HisrAcra4 antibodies did not neutralize any of the five scorpion venoms tested. However, an antibody blend of anti-HisrAcra4 and anti-HisrSccTx was able to neutralize A. crassicauda and A. mauritanicus venoms.

Conclusions: Two recombinant Nav neurotoxins, from different peptide families, were used as antigens to generate IgGs for neutralizing scorpion venoms of species from the Middle East and North Africa.

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雄蛾神经毒素两个肽家族的重组表达及抗原性研究。

背景:蝎子神经毒素，如那些改变哺乳动物电压门控钠离子通道(Nav)的毒素，是蝎子中毒的主要原因。它们的中和作用对于产生抗蝎子螫伤的抗蛇毒血清至关重要。方法:在本研究中，在大肠杆菌Origami中重组表达了两个计算机设计的基因，一个编码来自安纳托利亚蝎子(Androctonus crassicauda)毒液的天然神经毒素，命名为Acra 4，另一个非天然毒素，命名为共识蝎子毒素(SccTx)，从中东和北非蝎子最毒的神经毒素的初级结构中获得。结果:经细菌表达后，从包涵体中获得了两种表达的神经毒素，分别命名为HisrAcra4和HisrSccTx。两种重组神经毒素均以多种Cys-Cys亚型获得。重新折叠后的活性蛋白片段HisrAcra4和HisrSccTx的分子质量分别为8,947.6 Da和9,989.1 Da，与预期的理论质量一致。以HisrAcra4和HisrSccTx作为抗原免疫两组家兔，产生抗HisrAcra4或抗HisrSccTx血清抗体，进而识别和中和来自中东和北非蝎子毒液的神经毒素。兔源抗体对南方雄蛾、致倦雄蛾和虎眼Buthus occitanus毒液的3LD50均有中和作用，但对粗纹田鼠和毛利塔尼田鼠毒液的3LD50无中和作用。此外，抗hisracra4抗体不能中和测试的五种蝎子毒液中的任何一种。然而，抗hisracra4和抗hisrscctx的混合抗体能够中和A. crassicauda和A. mauritanicus毒液。结论:利用来自不同肽科的两种重组Nav神经毒素作为抗原，制备了免疫球蛋白(igg)，用于中和中东和北非蝎子毒液。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Venomous Animals and Toxins Including Tropical Diseases 医学-毒理学

CiteScore

4.80

自引率

8.30%

发文量

审稿时长

6-12 weeks

期刊介绍： Journal of Venomous Animals and Toxins including Tropical Diseases (JVATiTD) is a non-commercial academic open access publication dedicated to research on all aspects of toxinology, venomous animals and tropical diseases. Its interdisciplinary content includes original scientific articles covering research on toxins derived from animals, plants and microorganisms. Topics of interest include, but are not limited to:systematics and morphology of venomous animals;physiology, biochemistry, pharmacology and immunology of toxins;epidemiology, clinical aspects and treatment of envenoming by different animals, plants and microorganisms;development and evaluation of antivenoms and toxin-derivative products;epidemiology, clinical aspects and treatment of tropical diseases (caused by virus, bacteria, algae, fungi and parasites) including the neglected tropical diseases (NTDs) defined by the World Health Organization.

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