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通过IgG1单链的蛋白水解引导双特异性单价抗体形成。

Guiding bispecific monovalent antibody formation through proteolysis of IgG1 single-chain.

作者信息

Dimasi Nazzareno, Fleming Ryan, Sachsenmeier Kris F, Bezabeh Binyam, Hay Carl, Wu Jincheng, Sult Erin, Rajan Saravanan, Zhuang Li, Cariuk Peter, Buchanan Andrew, Bowen Michael A, Wu Herren, Gao Changshou

机构信息

a Antibody Discovery and Protein Engineering, MedImmune , Gaithersburg , MD , USA.

b Translational Sciences, IMED Oncology AstraZeneca , Waltham , MA , USA.

出版信息

MAbs. 2017 Apr;9(3):438-454. doi: 10.1080/19420862.2016.1277301. Epub 2017 Jan 5.

Abstract

We developed an IgG1 domain-tethering approach to guide the correct assembly of 2 light and 2 heavy chains, derived from 2 different antibodies, to form bispecific monovalent antibodies in IgG1 format. We show here that assembling 2 different light and heavy chains by sequentially connecting them with protease-cleavable polypeptide linkers results in the generation of monovalent bispecific antibodies that have IgG1 sequence, structure and functional properties. This approach was used to generate a bispecific monovalent antibody targeting the epidermal growth factor receptor and the type I insulin-like growth factor receptor that: 1) can be produced and purified using standard IgG1 techniques; 2) exhibits stability and structural features comparable to IgG1; 3) binds both targets simultaneously; and 4) has potent anti-tumor activity. Our strategy provides new engineering opportunities for bispecific antibody applications, and, most importantly, overcomes some of the limitations (e.g., half-antibody and homodimer formation, light chains mispairing, multi-step purification), inherent with some of the previously described IgG1-based bispecific monovalent antibodies.

摘要

我们开发了一种IgG1结构域连接方法,以引导源自两种不同抗体的两条轻链和两条重链正确组装,形成IgG1形式的双特异性单价抗体。我们在此表明,通过用蛋白酶可裂解的多肽接头依次连接两条不同的轻链和重链来进行组装,会产生具有IgG1序列、结构和功能特性的单价双特异性抗体。该方法用于生成一种靶向表皮生长因子受体和I型胰岛素样生长因子受体的双特异性单价抗体,其具有以下特点:1)可使用标准IgG1技术生产和纯化;2)表现出与IgG1相当的稳定性和结构特征;3)同时结合两个靶点;4)具有强大的抗肿瘤活性。我们的策略为双特异性抗体应用提供了新的工程学机会,最重要的是,克服了一些先前描述的基于IgG1的双特异性单价抗体所固有的局限性(例如,半抗体和同二聚体形成、轻链错配、多步纯化)。

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