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首页> 外文期刊>Methods: A Companion to Methods in Enzymology >Engineering therapeutic bispecific antibodies using CrossMab technology
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Engineering therapeutic bispecific antibodies using CrossMab technology

机译:使用Crossmab技术的工程治疗性双特异性抗体

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摘要

Bispecific antibodies have recently gained major interest as they allow novel mechanisms-of-action and/or therapeutic applications that cannot be achieved using conventional IgG-based antibodies. A major issue in engineering IgG-based bispecific antibodies has been to enable the correct association of heavy and light chains resulting in correct assembly of the desired bispecific antibody in sufficient yield. Various approaches have been described during recent years to tackle this challenge. We have developed the so-called CrossMab technology that enforces correct light chain association based on the domain crossover of immunoglobulin domains in the Fab region of the bispecific antibody. This versatile technology allows the generation of different bispecific antibody formats including asymmetric heterodimeric monovalent 1 + 1 bispecific antibodies and asymmetric heterodimeric bispecific antibodies with 2 + 1 valency in combination with approaches enabling Fc-hetermodimerization like knob-into-hole technology as well as the generation of tetravalent symmetric bispecific antibodies with 2 + 2 valency, also known as Tandem-Fab based IgG antibodies, using processes suitable for the large scale production of therapeutic bispecific antibodies. Notably, as of now, at least eight different bispecific antibodies using CrossMab technology entered clinical development, and additional CrossMabs are in late preclinical development. This review provides a summary of the status and progress with the engineering and generation of CrossMab technology based bispecific antibodies as well as their therapeutic application.
机译:双特异性抗体最近获得了主要利益,因为它们允许使用常规IgG基抗体无法实现的新的动作机制和/或治疗应用。工程基于IgG的双特异性抗体的主要问题已经能够以足够的产率来实现重型和轻链的正确组装,从而使所需的双特异性抗体正确组装。近年来已经描述了各种方法来解决这一挑战。我们已经开发了所谓的交叉组合技术,基于双特异性抗体的Fab区域中的免疫球蛋白结构域的域交叉来实施正确的轻链协会。这种多功能技术允许产生不同的双特异性抗体形式,包括不对称的异二二价一价1 + 1双特异性抗体和不对称的异二聚体双特异性抗体,其具有2 + 1个级的方法,与旋钮入孔技术等Fc-hetermodimerization的方法以及发电具有2 + 2个价的四价对称双特异性抗体,也称为基于串联的IgG抗体,使用适用于治疗性双特异性抗体的大规模生产的方法。值得注意的是,截至目前,使用Crossmab技术的至少八种不同的双特异性抗体进入临床开发,并且额外的横梁是晚期临床前发育。本综述提供了基于Bispecific抗体的横梁技术的工程和生成以及其治疗应用的状态和进展的摘要。

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