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评估抗肉毒杆菌寡克隆抗体制剂的协同中和作用。

Evaluating the synergistic neutralizing effect of anti-botulinum oligoclonal antibody preparations.

作者信息

Diamant Eran, Lachmi Bat-El, Keren Adi, Barnea Ada, Marcus Hadar, Cohen Shoshana, David Alon Ben, Zichel Ran

机构信息

Department of Biotechnology, Israel Institute for Biological Research, Ness Ziona, Israel.

Department of Infectious Diseases, Israel Institute for Biological Research, Ness Ziona, Israel.

出版信息

PLoS One. 2014 Jan 27;9(1):e87089. doi: 10.1371/journal.pone.0087089. eCollection 2014.

Abstract

Botulinum neurotoxins (BoNT) are considered some of the most lethal known substances. There are seven botulinum serotypes, of which types A, B and E cause most human botulism cases. Anti-botulinum polyclonal antibodies (PAbs) are currently used for both detection and treatment of the disease. However, significant improvements in immunoassay specificity and treatment safety may be made using monoclonal antibodies (MAbs). In this study, we present an approach for the simultaneous generation of highly specific and neutralizing MAbs against botulinum serotypes A, B, and E in a single process. The approach relies on immunization of mice with a trivalent mixture of recombinant C-terminal fragment (Hc) of each of the three neurotoxins, followed by a parallel differential robotic hybridoma screening. This strategy enabled the cloning of seven to nine MAbs against each serotype. The majority of the MAbs possessed higher anti-botulinum ELISA titers than anti-botulinum PAbs and had up to five orders of magnitude greater specificity. When tested for their potency in mice, neutralizing MAbs were obtained for all three serotypes and protected against toxin doses of 10 MsLD50-500 MsLD50. A strong synergistic effect of up to 400-fold enhancement in the neutralizing activity was observed when serotype-specific MAbs were combined. Furthermore, the highly protective oligoclonal combinations were as potent as a horse-derived PAb pharmaceutical preparation. Interestingly, MAbs that failed to demonstrate individual neutralizing activity were observed to make a significant contribution to the synergistic effect in the oligoclonal preparation. Together, the trivalent immunization strategy and differential screening approach enabled us to generate highly specific MAbs against each of the A, B, and E BoNTs. These new MAbs may possess diagnostic and therapeutic potential.

摘要

肉毒杆菌神经毒素(BoNT)被认为是已知最具致死性的物质之一。肉毒杆菌有七种血清型,其中A、B和E型导致了大多数人类肉毒中毒病例。抗肉毒杆菌多克隆抗体(PAbs)目前用于该疾病的检测和治疗。然而,使用单克隆抗体(MAbs)可能会显著提高免疫测定的特异性和治疗安全性。在本研究中,我们提出了一种在单个过程中同时产生针对肉毒杆菌A、B和E型血清型的高特异性中和单克隆抗体的方法。该方法依赖于用三种神经毒素各自的重组C末端片段(Hc)的三价混合物免疫小鼠,然后进行平行差异机器人杂交瘤筛选。这种策略使得能够针对每种血清型克隆出七到九个单克隆抗体。大多数单克隆抗体具有比抗肉毒杆菌多克隆抗体更高的抗肉毒杆菌ELISA效价,并且特异性高达五个数量级。在小鼠中测试其效力时,获得了针对所有三种血清型的中和单克隆抗体,并能抵御10 MsLD50 - 500 MsLD50的毒素剂量。当血清型特异性单克隆抗体组合时,观察到中和活性增强了高达400倍的强烈协同效应。此外,高度保护性的寡克隆组合与马源多克隆抗体制剂一样有效。有趣的是,未表现出个体中和活性的单克隆抗体被观察到对寡克隆制剂中的协同效应有显著贡献。总之,三价免疫策略和差异筛选方法使我们能够针对A、B和E型肉毒杆菌神经毒素各自产生高特异性的单克隆抗体。这些新的单克隆抗体可能具有诊断和治疗潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/40da/3903612/89f6fea72ae6/pone.0087089.g001.jpg

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