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An efficient route to the production of an IgG-like bispecific antibody.

机译:生产IgG类双特异性抗体的有效途径。

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摘要

Production of IgG-form bispecific antibody (BsAb-IgG) by co-expressing two antibodies in transfected cells is often inefficient owing to the unwanted pairing between the component heavy and light chains. We have developed an efficient method for the production of a novel IgG-like BsAb by using the natural dimerization mechanism between IgG heavy and light chains. Two single-chain Fv (scFv) of different specificity are fused to the constant domain of human kappa chain (C(L)) and the first constant domain of human heavy chain (C(H1)), to form two polypeptides, (scFv)(1)-C(L) and (scFv)(2)-C(H1)-C(H2)-C(H3), respectively. Co-expression of the two polypeptides in mammalian cells results in the formation of a covalently linked IgG-like hetero-tetramer, Bs(scFv)(4)-IgG, with dual specificity. Our approach yields a homogeneous bispecific IgG-like antibody product with each molecule containing four antigen binding sites, two for each of its target antigens. A Bs(scFv)(4)-IgG was prepared using two scFv antibodies each directed against a different epitope of a vascular endothelial growth factor receptor, the kinase insert domain-containing receptor (KDR). The Bs(scFv)(4)-IgG is capable of simultaneously binding to the two epitopes on the receptor. Further, the Bs(scFv)(4)-IgG also retains the antigen-binding efficacy and biological activity of its component antibodies.
机译:通过在转染的细胞中共表达两种抗体,IgG形式的双特异性抗体(BsAb-IgG)的生产通常效率低下,这是由于组分重链和轻链之间不需要的配对。我们已经开发出一种有效的方法,通过使用IgG重链和轻链之间的天然二聚化机理来生产新型IgG样BsAb。将两个不同特异性的单链Fv(scFv)融合到人kappa链的恒定域(C(L))和人重链的第一个恒定域(C(H1)),形成两个多肽(scFv )(1)-C(L)和(scFv)(2)-C(H1)-C(H2)-C(H3)。这两种多肽在哺乳动物细胞中的共表达导致形成具有双重特异性的共价连接的IgG样异四聚体Bs(scFv)(4)-IgG。我们的方法产生了均质的双特异性IgG样抗体产品,每个分子包含四个抗原结合位点,每个靶抗原都有两个。使用两种scFv抗体分别制备Bs(scFv)(4)-IgG,这些抗体分别针对血管内皮生长因子受体(包含激酶插入域的受体)(KDR)的不同表位。 Bs(scFv)(4)-IgG能够同时结合受体上的两个表位。此外,Bs(scFv)(4)-IgG还保留了其组成抗体的抗原结合功效和生物学活性。

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