Department of Biotechnology and Biomedicine, Technical University of Denmark, DK-2800, Kongens Lyngby, Denmark.
Instituto Clodomiro Picado, Facultad de Microbiologia, Universidad de Costa Rica, San Jose, Costa Rica.
Nat Commun. 2024 Jan 16;15(1):173. doi: 10.1038/s41467-023-42624-5.
Improved therapies are needed against snakebite envenoming, which kills and permanently disables thousands of people each year. Recently developed neutralizing monoclonal antibodies against several snake toxins have shown promise in preclinical rodent models. Here, we use phage display technology to discover a human monoclonal antibody and show that this antibody causes antibody-dependent enhancement of toxicity (ADET) of myotoxin II from the venomous pit viper, Bothrops asper, in a mouse model of envenoming that mimics a snakebite. While clinical ADET related to snake venom has not yet been reported in humans, this report of ADET of a toxin from the animal kingdom highlights the necessity of assessing even well-known antibody formats in representative preclinical models to evaluate their therapeutic utility against toxins or venoms. This is essential to avoid potential deleterious effects as exemplified in the present study.
需要改进治疗方法来对抗蛇咬伤中毒,每年有数千人因此死亡或永久残疾。最近开发的针对几种蛇毒素的中和单克隆抗体在临床前啮齿动物模型中显示出前景。在这里,我们使用噬菌体展示技术发现了一种人源单克隆抗体,并表明该抗体在模拟蛇咬伤的中毒小鼠模型中引起了来自毒蛇响尾蛇属的肌肉毒素 II 的抗体依赖性增强毒性(ADET)。虽然尚未在人类中报告与蛇毒相关的临床 ADET,但本报告中关于来自动物王国的毒素的 ADET 突出表明,即使是众所周知的抗体形式,也有必要在有代表性的临床前模型中进行评估,以评估其对毒素或毒液的治疗用途。这对于避免潜在的有害影响至关重要,正如本研究中所举例说明的那样。
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