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Variable heavy–variable light domain and Fab-arm CrossMabs with charged residue exchanges to enforce correct light chain assembly

机译:可变重可变轻域和带电荷残基交换的Fab臂CrossMab以强制正确的轻链组装

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摘要

Technologies for the production of bispecific antibodies need to overcome two major challenges. The first one is correct heavy chain assembly, which was solved by knobs-into-holes technology or charge interactions in the CH3 domains. The second challenge is correct light chain assembly. This can be solved by engineering the Fab-arm interfaces or applying the immunoglobulin domain crossover approach. There are three different crossovers possible, namely Fab-arm, constant domain and variable domain crossovers. The CrossMabCH1–CL exchange does not lead to the formation of unexpected side products, whereas the CrossMabFab and the CrossMabVH–VL formats result in the formation of typical side products. Thus, CrossMabCH1–CL was initially favored for therapeutic antibody development. Here, we report a novel improved CrossMab design principle making use of site-specific positional exchanges of charged amino acid pairs in the constant domain of these CrossMabs to enable the correct light chain assembly in the CrossMabVH–VL and improvements for the CrossMabFab design.
机译:生产双特异性抗体的技术需要克服两个主要挑战。第一个是正确的重链组装,这是通过旋钮入孔技术或CH3域中的电荷相互作用解决的。第二个挑战是正确的轻链组装。这可以通过设计Fab臂界面或应用免疫球蛋白域交叉方法来解决。可能有三种不同的交叉,即Fab臂,恒定域和可变域交叉。 CrossMab CH1-CL 交换不会导致意外的副产物形成,而CrossMab Fab 和CrossMab VH–VL 格式会导致在形成典型的副产品。因此,CrossMab CH1-CL 最初被认为可用于治疗性抗体的开发。在这里,我们报告了一种新颖的改良CrossMab设计原理,该原理利用这些CrossMab恒定域中带电氨基酸对的特定位置交换来实现CrossMab VH–VL 中的正确轻链组装和CrossMab Fab 设计的改进。

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