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首页> 外文期刊>Toxins >Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims ?
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Biosynthetic Oligoclonal Antivenom (BOA) for Snakebite and Next-Generation Treatments for Snakebite Victims ?

机译:用于蛇咬伤的生物合成寡克隆抗毒剂(BOA)和蛇咬伤受害者的下一代治疗方法?

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摘要

Snakebite envenoming is a neglected tropical disease that each year claims the lives of 80,000–140,000 victims worldwide. The only effective treatment against envenoming involves intravenous administration of antivenoms that comprise antibodies that have been isolated from the plasma of immunized animals, typically horses. The drawbacks of such conventional horse-derived antivenoms include their propensity for causing allergenic adverse reactions due to their heterologous and foreign nature, an inability to effectively neutralize toxins in distal tissue, a low content of toxin-neutralizing antibodies, and a complex manufacturing process that is dependent on husbandry and procurement of snake venoms. In recent years, an opportunity to develop a fundamentally novel type of antivenom has presented itself. By using modern antibody discovery strategies, such as phage display selection, and repurposing small molecule enzyme inhibitors, next-generation antivenoms that obviate the drawbacks of existing plasma-derived antivenoms could be developed. This article describes the conceptualization of a novel therapeutic development strategy for biosynthetic oligoclonal antivenom (BOA) for snakebites based on recombinantly expressed oligoclonal mixtures of human monoclonal antibodies, possibly combined with repurposed small molecule enzyme inhibitors.
机译:蛇咬毒害是一种被忽视的热带病,每年夺走全球80,000–140,000名受害者的生命。唯一有效的抗蛇毒治疗包括抗蛇毒血清的静脉内给药,该抗蛇毒血清包含已从免疫动物(通常是马)的血浆中分离出来的抗体。此类常规的源自马的抗蛇毒草的缺点包括由于其异源和外来性质而易于引起过敏性不良反应,无法有效中和远端组织中的毒素,毒素中和抗体的含量低以及制造过程复杂等缺点。依赖于蛇毒的饲养和采购。近年来,发展出一种从根本上新颖的抗蛇毒素的机会已经出现。通过使用现代抗体发现策略(例如噬菌体展示选择)和重新利用小分子酶抑制剂,可以开发出消除现有血浆来源抗蛇毒肽缺点的下一代抗蛇毒肽。本文介绍了基于人单克隆抗体重组表达的寡克隆混合物(可能与经过重新利用的小分子酶抑制剂组合)的蛇咬生物合成寡克隆抗蛇毒(BOA)新型治疗开发策略的概念。

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