Jinnyoung Choi (Agilent Technologies Korea)

Jinnyoung Choi (Agilent Technologies Korea)

Jinnyoung Choi (Agilent Technologies Korea)

Rachel Franklin (Agilent Technologies, Inc., Corvallis, OR, United States)

Julie Horner-Buxton (Agilent Technologies, Santa Clara, CA, United States)

Joseph C. Meeuwsen (Agilent Technologies, Inc., Corvallis, OR, United States)

Thomas E. Walker (Agilent Technologies, Lexington, MA, United States)

Mike Hare (Agilent Technologies, Inc., Corvallis, OR, United States)

Over the past few years, the demand for GLP-1 receptor agonists for managing type 2 diabetes and obesity has surged. As new GLP-1 receptor agonists emerge, characterizing primary sequence and modification identities early in the development cycle is crucial. In this study we demonstrate in-depth LC-MS/MS sequence and modification characterization of multiple GLP-1 receptor agonists. Electron capture dissociation (ECD) facilitated the detailed characterization of GLP-1 receptor agonists by generating sequence-informative fragments while retaining modifications1 . ExDViewer was applied to analyze fragmentation patterns of GLP-1 receptor agonists with non-standard building blocks and modifications.

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