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An exploratory universal LC-MS/MS assay for bioanalysis of hinge region-stabilized human IgG4 mAbs in clinical studies

机译:探索性通用LC-MS / MS测定法用于临床研究中铰链区稳定的人IgG4 mAb的生物分析

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摘要

Background: Due to the increasing number of monoclonal antibody (mAb) drug candidates entering clinical development, bioanalytical laboratories can benefit from generic liquid chromatography-tandem mass spectrometry (LC-MS/MS) assays capable of quantifying a variety of human mAb-based therapeutic drug candidates in plasma/serum samples from clinical studies. Results: We have developed and evaluated an exploratory LC-MS/MS assay capable of quantifying hinge region-stabilized IgG4 therapeutic mAb drugs and drug candidates in clinical samples. The exploratory assay is based upon a single 'universal IgG4 surrogate peptide. Conclusion: The novel exploratory LC-MS/MS assay reported herein, upon further refinement and full validation, is predicted to enable bioanalytical scientists to quantify all hinge region-stabilized human IgG4 therapeutic mAbs in human studies without having to develop a new assay for every new stabilized IgG4 mAb entering clinical development.
机译:背景:由于进入临床研究的单克隆抗体(mAb)候选药物的数量不断增加,生物分析实验室可以从通用液相色谱-串联质谱(LC-MS / MS)分析中受益,该分析能够量化多种基于人mAb的治疗药物临床研究中血浆/血清样品中的候选药物。结果:我们已经开发并评估了一种探索性LC-MS / MS分析方法,该方法能够量化铰链区稳定的IgG4治疗性mAb药物和临床样品中的候选药物。探索性测定基于单个'通用IgG4替代肽。结论:本文报道的新颖的探索性LC-MS / MS分析方法经过进一步完善和全面验证,预计将使生物分析科学家能够对人体研究中所有铰链区稳定的人IgG4治疗性mAb进行定量,而不必为每种方法开发新的分析方法新型稳定的IgG4 mAb进入临床开发。

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