Method Development for Reversed-Phase Separations of Peptides: A Rational Screening Strategy for Column and Mobile Phase Combinations with Complementary Selectivity

Author:

Field Jennifer K.1,Bruce James2,Buckenmaier Stephen3,Cheung Ming Yui4,Euerby Melvin R.1,Haselmann Kim F.5,Lau Jesper F.5,Stoll Dwight6,Sylvester Marie6,Thogersen Henning5,Petersson Patrik7

Affiliation:

1. Shimadzu

2. The Open University

3. Agilent Technologies

4. Oxford Nanopore Technologies

5. Novo Nordisk

6. Gustavus Adolphus College

7. Ferring Pharmaceuticals

Abstract

This review article summarizes the results obtained from the combined efforts of a joint academic and industrial initiative to solve the real-life challenge of determining low levels of peptide-related impurities (typically 0.05–1% of the drug substance) in the presence of the related biologically active peptide at a high concentration. A rational screening strategy for pharmaceutically important peptides has been developed that uses combinations of reversed‑phase ultrahigh-pressure liquid chromatography (UHPLC) columns and mobile phases that exhibit complementary reversed-phase chromatographic selectivity using either UV- or mass spectrometry (MS)-compatible conditions. Numerous stationary and mobile phases were categorized using the chemometric tool of principal component analysis (PCA), employing a novel characterization protocol utilizing specifically designed peptide probes. This was successfully applied to the development of a strategy for the detection of impurities (especially isomers) in peptide drug substances using two-dimensional liquid chromatography coupled with MS detection (2D-LC–MS).

Publisher

Multimedia Pharma Sciences, LLC

Subject

Analytical Chemistry

Reference20 articles.

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2. The top selling prescription drugs by revenue, accessed 24 Jan. 2022: https://www.pharmaceutical-technology.com/analysis/top-selling-prescription-drugs/

3. R.S. Rogers, N.S. Nightlinger, B. Livingston, P. Campbell, R. Bailey, and A. Balland, mAbs 7, 881–890 (2015).

4. J.K. Field, M.R. Euerby, P. Petersson, J. Lau, and H. Thøgersen, J. Chromatogr. A 1603, 113–129 (2019).

5. J.K. Field, M.R. Euerby, and P. Petersson, J. Chromatogr. A 1603, 102–112 (2019).

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