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使用卡宾化学足迹法对抗体结合表位进行残基水平表征。

Residue-Level Characterization of Antibody Binding Epitopes Using Carbene Chemical Footprinting.

作者信息

Hogan Jason M, Lee Peter S, Wong Susan C, West Sean M, Morishige Winse H, Bee Christine, Tapia Gamze Camdere, Rajpal Arvind, Strop Pavel, Dollinger Gavin

机构信息

Discovery Biotherapeutics, Bristol Myers Squibb, 700 Bay Road, Redwood City, California 94063, United States.

出版信息

Anal Chem. 2023 Feb 28;95(8):3922-3931. doi: 10.1021/acs.analchem.2c03091. Epub 2023 Feb 15.

Abstract

Characterization of antibody binding epitopes is an important factor in therapeutic drug discovery, as the binding site determines and drives antibody pharmacology and pharmacokinetics. Here, we present a novel application of carbene chemical footprinting with mass spectrometry for identification of antibody binding epitopes at the single-residue level. Two different photoactivated diazirine reagents provide complementary labeling information allowing structural refinement of the antibody binding interface. We applied this technique to map the epitopes of multiple MICA and CTLA-4 antibodies and validated the findings with X-ray crystallography and yeast surface display epitope mapping. The characterized epitopes were used to understand biolayer interferometry-derived competitive binding results at the structural level. We show that carbene footprinting provides fast and high-resolution epitope information critical in the antibody selection process and enables mechanistic understanding of function to accelerate the drug discovery process.

摘要

抗体结合表位的表征是治疗药物发现中的一个重要因素,因为结合位点决定并驱动抗体的药理学和药代动力学。在此,我们展示了一种将卡宾化学足迹法与质谱联用的新应用,用于在单残基水平鉴定抗体结合表位。两种不同的光活化重氮甲烷试剂提供互补的标记信息,有助于对抗体结合界面进行结构优化。我们应用该技术绘制了多种MICA和CTLA-4抗体的表位,并通过X射线晶体学和酵母表面展示表位图谱验证了研究结果。所表征的表位用于在结构层面理解生物层干涉术衍生的竞争性结合结果。我们表明,卡宾足迹法提供了在抗体筛选过程中至关重要的快速且高分辨率的表位信息,并能够从机制上理解功能,从而加速药物发现过程。

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