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鉴定抗肉毒神经毒素 A 的中和型鼠源人嵌合和改组抗体。

Characterization of neutralizing mouse-human chimeric and shuffling antibodies against botulinum neurotoxin A.

机构信息

Department of Veterinary Science, Graduate School of Life and Environmental Sciences, Osaka Prefecture University, 1-58, Rinku Orai-Kita, Izumisano, Osaka 598-8531, Japan.

出版信息

Microbiol Immunol. 2012 Nov;56(11):748-55. doi: 10.1111/j.1348-0421.2012.00503.x.

Abstract

Mouse-human chimeric monoclonal antibodies that could neutralize botulinum neurotoxins were developed and an attempt was made to establish mouse hybridoma cell clones that produced monoclonal antibodies that neutralized botulinum neurotoxin serotype A (BoNT/A). Four clones (2-4, 2-5, 9-4 and B1) were selected for chimerization on the basis of their neutralizing activity against BoNT/A and the cDNA of the variable regions of their heavy (V(H)) and light chains (V(L)) were fused with the upstream regions of the constant counterparts of human kappa light and gamma 1 heavy chain genes, respectively. CHO-DG44 cells were transfected with these plasmids and mouse-human chimeric antibodies (AC24, AC25, AC94 and ACB1) purified to examine their binding and neutralizing activities. Each chimeric antibody exhibited almost the same capability as each parent mouse mAb to bind and neutralize activities against BoNT/A. From the chimeric antibodies against BoNT/A, shuffling chimeric antibodies designed with replacement of their V(H) or V(L) domains were constructed. A shuffling antibody (AC2494) that derived its V(H) and V(L) domains from chimeric antibodies AC24 and AC94, respectively, showed much higher neutralizing activity than did other shuffling antibodies and parent counterparts. This result indicates that it is possible to build high-potency neutralizing chimeric antibodies by selecting and shuffling V(H) and V(L) domains from a variety of repertoires. A shuffling chimeric antibody might be the best candidate for replacing horse antitoxin for inducing passive immunotherapy against botulism.

摘要

研制了能够中和肉毒神经毒素的鼠人嵌合单克隆抗体,并试图建立产生中和肉毒神经毒素血清型 A(BoNT/A)的单克隆抗体的鼠杂交瘤细胞克隆。根据其对 BoNT/A 的中和活性,选择了 4 个克隆(2-4、2-5、9-4 和 B1)进行嵌合化,其重链(V(H))和轻链(V(L))的可变区的 cDNA 分别与人κ轻链和γ 1 重链基因的恒定区上游融合。用这些质粒转染 CHO-DG44 细胞,并纯化鼠人嵌合抗体(AC24、AC25、AC94 和 ACB1),以检查它们的结合和中和活性。每个嵌合抗体都表现出与各自亲本鼠 mAb 几乎相同的能力,能够结合和中和 BoNT/A 的活性。从针对 BoNT/A 的嵌合抗体中,构建了设计用其 V(H)或 V(L)结构域替换的 shuffling 嵌合抗体。一种 shuffling 抗体(AC2494),其 V(H)和 V(L)结构域分别来自嵌合抗体 AC24 和 AC94,显示出比其他 shuffling 抗体和亲本抗体更高的中和活性。这一结果表明,通过从各种库中选择和 shuffling V(H)和 V(L)结构域,构建高效中和嵌合抗体是可能的。一种 shuffling 嵌合抗体可能是替代马抗毒素用于诱导肉毒中毒被动免疫治疗的最佳候选物。

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