Pre-study and in-study validation of a size-exclusion chromatography method with different detection modes for the analysis of monoclonal antibody aggregates.

J Chromatogr B Analyt Technol Biomed Life Sci

Departamento de Ingeniería Química y Tecnología Farmacéutica, Facultad de Ciencias de la Salud-Sección Farmacia, Universidad de La Laguna, 38200, Tenerife, Spain.

Published: June 2016

AI Article Synopsis

  • Size exclusion chromatography (SEC) was used to study the aggregation of bevacizumab under thermal stress, including different detection methods like light-scattering (SEC/LS) and differential refractive-index detection (SEC/RI).
  • The validation processes for these detection methods involved quality control samples and adherence to established guidelines to ensure reliable results.
  • The aggregation kinetics were analyzed using a modified Lumry-Eyring model, confirming a linear relationship with temperature, although the method's predictions varied at lower temperatures, highlighting the need for real-time stability assessments for product shelf-life.

Article Abstract

Size exclusion chromatography (SEC) with different detection modes was assessed as a means to characterize the type of bevacizumab aggregate that forms under thermal stress, quantitatively monitoring the aggregation kinetics. The combination of SEC with light-scattering (SEC/LS) detection was validated using in-study validation process. This was performed by applying a strategy based on a control chart to monitor the process parameters and by inserting quality control samples in routine runs. The SEC coupled with a differential refractive-index detector (SEC/RI) was validated using a pre-study validation process in accordance with the ICH-Q2 (R1) guidelines and in-study monitoring in accordance with the Analytical Target Profile (ATP) criteria. The total error and β-expectation tolerance interval rules were used to assess method suitability and control the risk of incorrectly accepting unsuitable analytical methods. The aggregation kinetics data were interpreted using a modified Lumry-Eyring model. The true order of the reaction was determined using the initial-rate approach. All the kinetic data show a linear Arrhenius dependence within the studied temperature range. The Arrhenius approach over-predicted the aggregation rate for 5°C, but provides an idea of the aggregation process and amount of aggregate formed. In any case, real-time stability data are necessary to establish the product shelf-life.

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http://dx.doi.org/10.1016/j.jchromb.2016.04.022DOI Listing

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