High-throughput untargeted screening of biotherapeutic macromolecules in equine plasma by UHPLC-HRMS/MS: Application to monoclonal antibodies and Fc-fusion proteins for doping control

IF 2.6 3区医学 Q2 BIOCHEMICAL RESEARCH METHODS Drug Testing and Analysis Pub Date : 2023-06-20 DOI:10.1002/dta.3525

Justine Pinetre, Vivian Delcourt, François Becher, Patrice Garcia, Agnès Barnabé, Benoit Loup, Marie-Agnès Popot, François Fenaille, Ludovic Bailly-Chouriberry

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Abstract

Many innovative biotherapeutics have been marketed in the last decade. Monoclonal antibodies (mAbs) and Fc-fusion proteins (Fc-proteins) have been developed for the treatment of diverse diseases (cancer, autoimmune diseases, and inflammatory disorders) and now represent an important part of targeted therapies. However, the ready availability of such biomolecules, sometimes characterized by their anabolic, anti-inflammatory, or erythropoiesis-stimulating properties, raises concerns about their potential misuse as performance enhancers for human and animal athletes. In equine doping control laboratories, a method has been reported to detect the administration of a specific human biotherapeutic in equine plasma; but no high-throughput method has been described for the screening without any a priori knowledge of human or murine biotherapeutic. In this context, a new broad-spectrum screening method involving UHPLC-HRMS/MS has been developed for the untargeted analysis of murine or human mAbs and related macromolecules in equine plasma. This approach, consisting of a “pellet digestion” strategy performed in a 96-well plate, demonstrates reliable performances at low concentrations (pmol/mL range) with high-throughput capability (≈100 samples/day). Targeting species-specific proteotypic peptides located within the constant parts of mAbs enables the “universal” detection of human biotherapeutics only by monitoring 10 peptides. As proof of principle, this strategy successfully detected different biotherapeutics in spiked plasma samples, and allowed, for the first time, the detection of a human mAb up to 10 days after a 0.12 mg/kg administration to a horse. This development will expand the analytical capabilities of horse doping control laboratories towards protein-based biotherapeutics with adequate sensitivity, throughput, and cost-effectiveness.

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利用超高效液相色谱-质谱联用仪（UHPLC-HRMS/MS）对马血浆中的生物治疗大分子进行高通量非靶向筛选：应用于兴奋剂控制中的单克隆抗体和 Fc 融合蛋白。

在过去的十年中，许多创新的生物治疗药物已经上市。单克隆抗体（mAbs）和 Fc 融合蛋白（Fc 蛋白）已被开发用于治疗多种疾病（癌症、自身免疫性疾病和炎症性疾病），目前已成为靶向疗法的重要组成部分。然而，此类生物大分子（有时具有合成代谢、抗炎或刺激红细胞生成的特性）的随时可用性引起了人们对其作为人类和动物运动员成绩提高剂的潜在滥用的担忧。据报道，在马兴奋剂控制实验室中，有一种方法可以检测马血浆中特定人类生物治疗剂的用量；但目前还没有描述过在对人类或鼠类生物治疗剂没有任何先验知识的情况下进行筛查的高通量方法。在这种情况下，我们开发了一种新的超高效液相色谱-质谱联用（UHPLC-HRMS/MS）广谱筛选方法，用于对马血浆中的鼠源性或人源性 mAbs 及相关大分子进行非靶向分析。这种方法包括在 96 孔板中执行 "颗粒消化 "策略，在低浓度（pmol/mL 范围内）和高通量能力（≈100 样品/天）条件下表现出可靠的性能。以位于 mAbs 恒定部分的物种特异性蛋白肽为目标，只需监测 10 个肽就能 "通用 "检测人类生物治疗药物。作为原理验证，这一策略成功地检测出了加标血浆样本中的不同生物治疗药物，并首次实现了在给马注射 0.12 毫克/千克的剂量后 10 天内检测出人类 mAb。这一研发成果将拓展马匹兴奋剂检测实验室的分析能力，使其能够以足够的灵敏度、处理量和成本效益检测以蛋白质为基础的生物治疗药物。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Drug Testing and Analysis BIOCHEMICAL RESEARCH METHODS-CHEMISTRY, ANALYTICAL

CiteScore

5.90

自引率

24.10%

发文量

191

审稿时长

2.3 months

期刊介绍： As the incidence of drugs escalates in 21st century living, their detection and analysis have become increasingly important. Sport, the workplace, crime investigation, homeland security, the pharmaceutical industry and the environment are just some of the high profile arenas in which analytical testing has provided an important investigative tool for uncovering the presence of extraneous substances. In addition to the usual publishing fare of primary research articles, case reports and letters, Drug Testing and Analysis offers a unique combination of; ‘How to’ material such as ‘Tutorials’ and ‘Reviews’, Speculative pieces (‘Commentaries’ and ‘Perspectives'', providing a broader scientific and social context to the aspects of analytical testing), ‘Annual banned substance reviews’ (delivering a critical evaluation of the methods used in the characterization of established and newly outlawed compounds). Rather than focus on the application of a single technique, Drug Testing and Analysis employs a unique multidisciplinary approach to the field of controversial compound determination. Papers discussing chromatography, mass spectrometry, immunological approaches, 1D/2D gel electrophoresis, to name just a few select methods, are welcomed where their application is related to any of the six key topics listed below.