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Isolation of TGF-beta-neutralizing single-domain antibodies of predetermined epitope specificity using next-generation DNA sequencing

机译:使用下一代DNA测序分离具有预定表位特异性的TGF-β中和单结构域抗体

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摘要

The epitope specificity of therapeutic antibodies is often critical to their efficacy and mode of action. Here, we report the isolation of single-domain antibodies (sdAbs) against a pre-specified epitope of TGF-beta 3: namely, the site of interaction between the cytokine and its cell-surface type II receptor. By panning a phage-displayed immune llama VhH library against TGF-beta 3 using competitive elution with soluble dimeric type II receptor ectodomain in tandem with next-generation DNA sequencing, we identified several sdAbs that competed with the receptor for TGF-beta 3 binding and neutralized TGF-beta 3 in in vitro cellular assays. In contrast, all other sdAbs identified using conventional panning approaches (i.e., without regard to epitope specificity) did not target the site of receptor:cytokine interaction. We expect this strategy to be generally applicable for identifying epitope-specific sdAbs when binding reagents directed against the epitope of interest are available. The sdAbs identified here are of potential interest as cancer immunotherapeutics.
机译:治疗性抗体的表位特异性通常对其功效和作用方式至关重要。在这里,我们报告了针对TGF-β3预先指定的表位的单域抗体(sdAbs)的分离:即细胞因子与其细胞表面II型受体之间相互作用的位点。通过使用可溶性二聚体II型受体胞外域与下一代DNA测序串联竞争洗脱淘选针对TGF-β3的噬菌体展示的免疫美洲驼VhH文库,我们鉴定了几种与该受体竞争TGF-β3结合的sdAb,并且在体外细胞试验中中和了TGF-beta 3。相反,使用常规淘选方法(即不考虑表位特异性)鉴定的所有其他sdAb均不靶向受体:细胞因子相互作用的位点。当可获得针对目的表位的结合试剂时,我们期望该策略通常可用于鉴定表位特异性sdAb。此处鉴定的sdAb作为癌症免疫疗法具有潜在的意义。

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