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Investigation of native and aggregated therapeutic proteins in human plasma with asymmetrical flow field-flow fractionation and mass spectrometry

Ingrid Ramm, Mats Leeman, Herje Schagerlöf, Ileana R. León, Alejandra Castro, Lars Nilsson

2022Analytical and Bioanalytical Chemistry14 citationsDOIOpen Access PDF

Abstract

Physiochemical degradation of therapeutic proteins in vivo during plasma circulation after administration can have a detrimental effect on their efficacy and safety profile. During drug product development, in vivo animal studies are necessary to explore in vivo protein behaviour. However, these studies are very demanding and expensive, and the industry is working to decrease the number of in vivo studies. Consequently, there is considerable interest in the development of methods to pre-screen the behaviour of therapeutic proteins in vivo using in vitro analysis. In this work, asymmetrical flow field-flow fractionation (AF4) and liquid chromatography-mass spectrometry (LC-MS) were combined to develop a novel analytical methodology for predicting the behaviour of therapeutic proteins in vivo. The method was tested with two proteins, a monoclonal antibody and a serum albumin binding affibody. After incubation of the proteins in plasma, the method was successfully used to investigate and quantify serum albumin binding, analyse changes in monoclonal antibody size, and identify and quantify monoclonal antibody aggregates.

Topics & Concepts

In vivoChemistryMonoclonal antibodyBlood proteinsAlbuminMass spectrometryChromatographyIn vitroFractionationSerum albuminAntibodyBiochemistryBiologyImmunologyBiotechnologyField-Flow Fractionation Techniquesthermodynamics and calorimetric analysesProtein purification and stability
Investigation of native and aggregated therapeutic proteins in human plasma with asymmetrical flow field-flow fractionation and mass spectrometry | Litcius