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An antibody with Fab-constant domains exchanged for a pair of CH3 domains

机译:与一对CH3结构域交换的Fab恒定结构域的抗体

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摘要

We have designed a complete antibody-like construct where the CH1 and Cκ domains are exchanged for a pair of the CH3 domains and efficient pairing of the heavy and light variable domain is achieved using "Knobs-into-Holes" strategy. This construct, composed of only naturally occurring immunoglobulin sequences without artificial linkers, expressed at a high level in mammalian cells, however exhibited low solubility. Rational mutagenesis aimed at the amino acid residues located at the interface of the variable domains and the exchanged CH3 domains was applied to improve the biophysical properties of the molecule. The domain-exchanged construct, including variable domains of the HER2/neu specific antibody trastuzumab, was able to bind to the surface of the strongly HER2/neu positive cell line SK-BR3 4-fold weaker than trastuzumab, but could nevertheless incite a more potent response in an antibody-dependent cell cytotoxicity (ADCC) reporter assay with FcγRIIIa-overexpressing T-cells. This could be explained with a stronger binding to the FcγRIIIa. Importantly, the novel construct could mediate a specific ADCC effect with natural killer cells similar to the parental antibody.
机译:我们设计了一种完整的抗体样构造,其中CH1和CK域被交换为一对CH3结构域,并且使用“旋钮 - 进入孔”策略实现重和光可变结构域的有效配对。然而,这种构造仅由没有人造接头的天然存在的免疫球蛋白序列组成,但在哺乳动物细胞中的高水平表达,但表现出低溶解度。施用旨在诱变位于可变结构域的界面和交换的CH3结构域的氨基酸残基的诱变以改善分子的生物物理性质。域交换的构建体,包括Her2 / Neu特异性抗体曲妥珠单抗的可变结构域,能够与强烈的HER2 / NEU阳性细胞系SK-BR3 4倍的表面结合,但尽管可以煽动更多抗体依赖性细胞细胞毒性(ADCC)报告试验用FcγRIIIA过表达T细胞进行有效响应。这可以用更强的结合对FcγRIIIA来解释。重要的是,新颖的构建体可以用与亲本抗体类似的自然杀伤细胞介导特异性ADCC效应。

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