Investigation of the Solid-State Interactions in Lyophilized Human G-CSF Using Hydrogen–Deuterium Exchange Mass Spectrometry

氢-氘交换 化学 质谱法 单体 赋形剂 色谱法 去酰胺 结晶学 生物物理学 生物化学 聚合物 有机化学 量子力学 生物 物理
作者
Victoria E. Wood,Mark-Adam W. Kellerman,Kate Groves,Milena Quaglia,Elizabeth M. Topp,Paul Matejtschuk,Paul A. Dalby
出处
期刊:Molecular Pharmaceutics [American Chemical Society]
卷期号:21 (4): 1965-1976 被引量:2
标识
DOI:10.1021/acs.molpharmaceut.3c01211
摘要

Hydrogen/deuterium exchange mass spectrometry (HDX-MS) previously elucidated the interactions between excipients and proteins for liquid granulocyte colony stimulating factor (G-CSF) formulations, confirming predictions made using computational structure docking. More recently, solid-state HDX mass spectrometry (ssHDX-MS) was developed for proteins in the lyophilized state. Deuterium uptake in ssHDX-MS has been shown for various proteins, including monoclonal antibodies, to be highly correlated with storage stability, as measured by protein aggregation and chemical degradation. As G-CSF is known to lose activity through aggregation upon lyophilization, we applied the ssHDX-MS method with peptide mapping to four different lyophilized formulations of G-CSF to compare the impact of three excipients on local structure and exchange dynamics. HDX at 22 °C was confirmed to correlate well with the monomer content remaining after lyophilization and storage at -20 °C, with sucrose providing the greatest protection, and then phenylalanine, mannitol, and no excipient leading to progressively less protection. Storage at 45 °C led to little difference in final monomer content among the formulations, and so there was no discernible relationship with total deuterium uptake on ssHDX. Incubation at 45 °C may have led to a structural conformation and/or aggregation mechanism no longer probed by HDX at 22 °C. Such a conformational change was observed previously at 37 °C for liquid-formulated G-CSF using NMR. Peptide mapping revealed that tolerance to lyophilization and -20 °C storage was linked to increased stability in the small helix, loop AB, helix C, and loop CD. LC-MS HDX and NMR had previously linked loop AB and loop CD to the formation of a native-like state (N*) prior to aggregation in liquid formulations, suggesting a similar structural basis for G-CSF aggregation in the liquid and solid states.
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