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Isomerization and Oxidation in the Complementarity-Determining Regions of a Monoclonal Antibody: A Study of the Modification-Structure-Function Correlations by Hydrogen-Deuterium Exchange Mass Spectrometry

机译:单克隆抗体互补决定区中的异构化和氧化:氢-氘交换质谱法对修饰-结构-功能相关性的研究

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Chemical modifications can potentially change monoclonal antibody's (mAb) local or global conformation and therefore impact their efficacy as therapeutic drugs. Modifications in the complementarity-determining regions (CDRs) are especially important because they can impair the binding affinity of an antibody for its target and therefore drug potency as a result. In order to understand the impact on mAb attributes induced by specific chemical modifications within the CDR, hydrogen deuterium exchange mass spectrometry (HDX MS) was used to interrogate the conformational impact of Asp isomerization and Met oxidation in the CDRs of a model monoclonal antibody (mAbl). Our results indicate that despite their proximity to each other, Asp54 isomerization and Met56 Oxidation in CDR2 in the heavy chain of mAbl result in opposing conformational impacts on the local and nearby regions, leading directly to different alterations on antibody antigen binding affinity. This study revealed direct evidence of local and global conformational changes caused by two of the most common degradation pathways in the CDRs of a mAb and identified correlations between chemical modification, structure, and function of the therapeutic monoclonal antibody.
机译:化学修饰可能会改变单克隆抗体(mAb)的局部或整体构象,因此会影响其作为治疗药物的功效。互补决定区(CDR)中的修饰特别重要,因为它们会损害抗体对其靶标的结合亲和力,从而削弱药物的效力。为了了解CDR中特定化学修饰对mAb属性的影响,使用氢氘交换质谱(HDX MS)来研究模型单克隆抗体(mAbl的CDR)中Asp异构化和Met氧化的构象影响)。我们的结果表明,尽管它们彼此接近,但mAb1重链中CDR2中的Asp54异构化和Met56氧化导致对局部和附近区域的构象相反,直接导致抗体抗原结合亲和力的不同改变。这项研究揭示了mAb CDR中两个最常见的降解途径引起的局部和全局构象变化的直接证据,并确定了治疗性单克隆抗体的化学修饰,结构和功能之间的相关性。

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