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

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

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...

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Published in:Drug testing and analysis Vol. 16; no. 2; pp. 199 - 209
Main Authors: Pinetre, Justine, Delcourt, Vivian, Becher, François, Garcia, Patrice, Barnabé, Agnès, Loup, Benoit, Popot, Marie‐Agnès, Fenaille, François, Bailly‐Chouriberry, Ludovic
Format: Journal Article
Language:English
Published: England Wiley Subscription Services, Inc 01-02-2024
John Wiley
Subjects:
Animals
Antibodies, Monoclonal
Chromatography, High Pressure Liquid - methods
Doping in Sports - prevention & control
equine doping control
Horses
Humans
Laboratories
Life Sciences
mAbs
Mice
Monoclonal antibodies
Peptides
Plasma
Proteins
targeted‐proteomics
UHPLC‐HRMS/MS
UHPLC-HRMS/MS
targeted-proteomics
equine doping control
mAbs
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Summary: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. Innovative biotherapeutics such as monoclonal antibodies (mAbs) and Fc‐fusion proteins have emerged as important targeted therapies for various diseases. However, concerns about their potential misuse as performance enhancers have led to the development of a high‐throughput method using UHPLC‐HRMS/MS, enabling the detection of human and murine mAbs in equine plasma.
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ISSN:1942-7603
1942-7611
DOI:10.1002/dta.3525