Synthetic glycopolymers as modulators of protein aggregation: influences of chemical composition, topology and concentration

Novel drug excipients are required to achieve stable formulations of protein drug candidates. Synthetic glycopolymers have been shown in some cases to improve protein formulation stability, although their structure-function relationship remains unknown. Here we report the synthesis of linear or 4-ar...

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Bibliographic Details
Published in:Journal of materials chemistry. B, Materials for biology and medicine Materials for biology and medicine, 2018, Vol.6 (7), p.1044-1054
Main Authors: Madeira do O, J, Mastrotto, F, Francini, N, Allen, S, van der Walle, C F, Stolnik, S, Mantovani, G
Format: Article
Language:English
Subjects:
Agglomeration
Amines
Arabinose
Astrochemistry
Carbohydrates
Chemical composition
Chemical synthesis
Drug development
Fab
Formulations
Galactose
Glucosamine
Glycopolymers
Lactose
Mannose
Modulation
Modulators
Monoclonal antibodies
Protein interaction
Proteins
Saccharides
Stress concentration
Structural stability
Structure-function relationships
Sugar
Temperature effects
Topology
Transition temperature
Transition temperatures
Trehalose
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Summary:Novel drug excipients are required to achieve stable formulations of protein drug candidates. Synthetic glycopolymers have been shown in some cases to improve protein formulation stability, although their structure-function relationship remains unknown. Here we report the synthesis of linear or 4-arm star glycopolymers with different molecular topology and chemical composition, with mannose, galactose, arabinose, N-acetyl glucosamine, lactose and trehalose pendant units - and investigate their modulation of conformational stability and aggregation propensity of a model monoclonal antibody (mAb1). Mono-and di-saccharides with free reducing ends are not frequently utilised as protein stabilisers, due to potential reactivity with protein's amine group. In this study, this was circumvented through the use of a stable acetal linker connecting the polymer backbone to the sugar pendant residues, which made the latter virtually non-reactive with amines. The general destabilisation of the antibody was determined as an unfolding transition temperature (T ) of CH and Fab structural domains, and aggregation temperature (T ). The most prominent effect of the glycopolymers on a temperature induced stress in low concentration solutions was a decrease in T and T , regardless of the sugar composition or glycopolymer topology - in contrast to the stabilising effect of the corresponding mono- and di-saccharide constituents. The exceptions of linear-lactose and star-trehalose glycopolymers, which increased T of the mAb Fab region and T , however, highlight a more complex structure-function relationship. Accelerated stability studies of the highly concentrated mAb solutions (50 mg mL ) revealed that the increased glycopolymer concentrations generally decreased the mAb stability, as judged by the amount of mAb1 'monomer' molecules in solution, with star- and linear-trehalose glycopolymers further generating visible aggregates. Interestingly the latter effect could not have been predicted from the T or T experiments conducted in a low concentration regime. Taken together, the data demonstrate the influence of a complex interplay of sugar chemistry and molecular topology of the synthetic glycopolymers on their modulation of protein conformational stability and aggregation propensity. The solution concentration was also an important parameter contributing to the stability modulation, and suggests that the stabilising properties of a sugar as a mono- or di-saccharide cannot be extr
ISSN:2050-750X
2050-7518
DOI:10.1039/c7tb02720f