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Kinetic mechanism of controlled Fab-arm exchange for the formation of bispecific immunoglobulin G1 antibodies

机译:受控Fab臂交换形成双特异性免疫球蛋白G1抗体的动力学机制

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摘要

Bispecific antibodies (bsAbs) combine the antigen specificities of two distinct Abs and demonstrate therapeutic promise based on novel mechanisms of action. Among the many platforms for creating bsAbs, controlled Fab-arm exchange (cFAE) has proven useful based on minimal changes to native Ab structure and the simplicity with which bsAbs can be formed from two parental Abs. Despite a published protocol for cFAE and its widespread use in the pharmaceutical industry, the reaction mechanism has not been determined. Knowledge of the mechanism could lead to improved yields of bsAb at faster rates as well as foster adoption of process control. In this work, a combination of Förster resonance energy transfer (FRET), nonreducing SDS-PAGE, and strategic mutation of the Ab hinge region was employed to identify and characterize the individual steps of cFAE. Fluorescence correlation spectroscopy (FCS) was used to determine the affinity of parental (homodimer) and bispecific (heterodimer) interactions within the CH3 domain, further clarifying the thermodynamic basis for bsAb formation. The result is a clear sequence of events with rate constants that vary with experimental conditions, where dissociation of the K409R parental Ab into half-Ab controls the rate of the reaction.
机译:双特异性抗体(bsAbs)结合了两种不同Abs的抗原特异性,并基于新的作用机制证明了治疗前景。在创建bsAb的众多平台中,基于对天然Ab结构的最小变化以及由两个亲本Abs形成bsAb的简单性,受控Fab臂交换(cFAE)已被证明是有用的。尽管已发布了有关cFAE的协议及其在制药工业中的广泛应用,但尚未确定反应机理。对该机制的了解可以提高bsAb的产率,并且速度更快,并促进过程控制的采用。在这项工作中,Förster共振能量转移(FRET),非还原SDS-PAGE和Ab铰链区的战略突变相结合,用于鉴定和表征cFAE的各个步骤。荧光相关光谱法(FCS)用于确定CH3域内的亲本(同二聚体)和双特异性(异二聚体)相互作用的亲和力,从而进一步阐明bsAb形成的热力学基础。结果是清晰的事件序列,其速率常数随实验条件而变化,其中K409R亲本Ab的解离成半Ab控制了反应速率。

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