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用于 IgG4 单克隆抗体构象表征的Native Mass Spectrometry、离子淌度和碰撞诱导解折叠。

Native Mass Spectrometry, Ion Mobility, and Collision-Induced Unfolding for Conformational Characterization of IgG4 Monoclonal Antibodies.

机构信息

Laboratoire de Spectrométrie de Masse BioOrganique , Université de Strasbourg, CNRS , IPHC UMR 7178 , 67000 Strasbourg , France.

IRPF - Centre d'Immunologie Pierre-Fabre (CIPF) , 74160 Saint-Julien-en-Genevois , France.

出版信息

Anal Chem. 2018 Aug 7;90(15):8865-8872. doi: 10.1021/acs.analchem.8b00912. Epub 2018 Jul 16.

DOI:10.1021/acs.analchem.8b00912
PMID:29956914
Abstract

Although the majority of FDA and EMA approved therapeutic monoclonal antibodies (mAbs) are IgG1, the number of IgG4-based formats reaching the market is increasing. IgG4 differs from other mAb isotypes by its specificity to form half mAbs that recombine into bispecific (bsAbs) molecules, through a process termed fab-arm exchange (FAE). We report here the complementarity of native mass spectrometry (MS), ion mobility (IM), and collision-induced unfolding (CIU) experiments for the structural characterization of members of the IgG4 subfamily (wild-type (wt), hinge-stabilized (hs, S228P mutation), and the resulting bsAb IgG4s). Native MS allows confirming/invalidating the occurrence of FAE as a function of these different types of IgG4. While IM-MS was unable to distinguish iso-cross-section IgG4 species, CIU experiments provide unique specific structural signatures of each individual IgG4 based on their specific unfolding pathways. Common CIU features of IgG4 formats include the observation of three conformational states and two transitions. In addition, CIU experiments demonstrated that S228P mutation stabilizes gas phase conformations of hsIgG4, in agreement with increased stability related to more rigid hinge regions. CIU patterns also appear to be more informative than IM-MS for bsAb structural characterization, unfolding signature of the bsAb being intermediate to the ones of the former parent wt-IgG4s, highlighting that bsAb CIU profiles keep the memory of their origins. Altogether, our results demonstrate that CIU patterns can serve as mAb specific structural signatures and are mature to be included in MS-based analytical workflows for conformational/structural characterization of mAb formats in early development phases and for multiple attribute monitoring.

摘要

尽管大多数 FDA 和 EMA 批准的治疗性单克隆抗体(mAb)是 IgG1,但基于 IgG4 的格式数量正在增加。与其他 mAb 同种型不同,IgG4 特异性地形成半抗体,通过称为 Fab-臂交换(FAE)的过程重组为双特异性(bsAb)分子。我们在此报告天然质谱(MS)、离子淌度(IM)和碰撞诱导解折叠(CIU)实验的互补性,用于 IgG4 亚家族成员(野生型(wt)、铰链稳定(hs,S228P 突变)和由此产生的 bsAb IgG4)的结构表征。天然 MS 允许根据这些不同类型的 IgG4 确认/验证 FAE 的发生。虽然 IM-MS 无法区分等交叉面积 IgG4 物种,但 CIU 实验基于其特定的展开途径,为每个 IgG4 提供独特的特定结构特征。IgG4 格式的常见 CIU 特征包括观察到三种构象状态和两个转变。此外,CIU 实验表明,S228P 突变稳定了 hsIgG4 的气相构象,这与更刚性铰链区域相关的增加稳定性一致。CIU 模式似乎也比 IM-MS 更能提供 bsAb 结构特征,bsAb 的展开特征介于前体 wt-IgG4s 之间,突出了 bsAb 的 CIU 谱保留了它们起源的记忆。总之,我们的结果表明,CIU 模式可以作为 mAb 特异性结构特征,并在基于 MS 的分析工作流程中成熟,用于 mAb 格式在早期开发阶段的构象/结构表征和多属性监测。

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