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A Single Tri-Epitopic Antibody Virtually Recapitulates the Potency of a Combination of Three Monoclonal Antibodies in Neutralization of Botulinum Neurotoxin Serotype A

机译:单个三齿抗体几乎重新承载三种单克隆抗体组合中和肉毒杆菌神经毒素血清型A的组合效力

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摘要

The standard of treatment for botulism, equine antitoxin, is a foreign protein with associated safety issues and a short serum half-life which excludes its use as a prophylactic antitoxin and makes it a less-than-optimal therapeutic. Due to these limitations, a recombinant monoclonal antibody (mAb) product is preferable. It has been shown that combining three mAbs that bind non-overlapping epitopes leads to highly potent botulinum neurotoxin (BoNT) neutralization. Recently, a triple human antibody combination for BoNT/A has demonstrated potent toxin neutralization in mouse models with no serious adverse events when tested in a Phase I clinical trial. However, a triple antibody therapeutic poses unique development and manufacturing challenges. Thus, potentially to streamline development of BoNT antitoxins, we sought to achieve the potency of multiple mAb combinations in a single IgG-based molecule that has a long serum half-life. The design, production, and testing of a single tri-epitopic IgG1-based mAb (TeAb) containing the binding sites of each of the three parental BoNT/A mAbs yielded an antibody of nearly equal potency to the combination. The approach taken here could be applied to the design and creation of other multivalent antibodies that could be used for a variety of applications, including toxin elimination.
机译:肉毒株(马抗毒素)的治疗标准是外国蛋白质,其具有相关的安全问题和短的血清半衰期,其用作预防性抗毒素的用途,使其成为较低的治疗性。由于这些限制,优选重组单克隆抗体(MAB)产物。已经表明,将三种MAb组合结合非重叠表位导致高度有效的肉毒杆菌神经毒素(BONT)中和。最近,对骚乱/ A的三重人抗体组合在小鼠模型中表现出有效的毒素中和,在I期临床试验中测试时没有严重不良事件。然而,三重抗体治疗姿势造成独特的发展和制造挑战。因此,潜在地简化逆毒素的发展,我们试图在具有长血清半衰期的单个IgG的分子中实现多种MAB组合的效力。含有三个亲本突发/ mAb中的每种粘合位点的单一三齿型IgG1的MAb(Temb)的设计,生产和测试产生了对组合具有几乎相等效力的抗体。这里采取的方法可以应用于可用于各种应用的其他多价抗体的设计和创造,包括毒素消除。

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