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Temperature-Switchable Glycopolymers and Their Conformation-Dependent Binding to Receptor Targets. | LitMetric

Temperature-Switchable Glycopolymers and Their Conformation-Dependent Binding to Receptor Targets.

Biomacromolecules

Institute of Organic and Macromolecular Chemistry, Heinrich-Heine-University Düsseldorf, Universitätsstraße 1, Dusseldorf 40225, Germany.

Published: July 2020

AI Article Synopsis

Article Abstract

The temperature-dependent binding of copolymers from poly(-isopropylacrylamide) (PNIPAM) and mannose ligands to and concanavalin A (ConA) is determined. Through polymer analogous reactions using poly(-acryloxysuccinimide) and amine-linked mannose residues with different linkers, glycopolymers are prepared with the variation of the mannose density. Quantitative adhesion inhibition assays show the inhibitory potential of the glycopolymers as a function of the mannose/NIPAM ratio and linker type above and below their lower critical solution temperature (LCST). Intriguingly, opposite temperature effects on the binding to and ConA are observed. While the inhibition is stronger above the LCST, the ConA inhibition is, in overall, weaker at elevated temperatures. When going beyond the LCST, the polymers undergo a coil-to-globule transition, forming microphases with surface-enriched hydrophilic sugar moieties exhibiting increased inhibition through steric shielding. However, the formation of such microphases above the LCST renders a fraction of carbohydrate ligands inaccessible,and the polymers remaining in the solution phase then have coil sizes below the minimum binding site spacing of the ConA receptor, explaining reduced ConA inhibition. Overall, these results suggest that the coil-to-globule transition of glycopolymers may induce lower or higher inhibitory potentials due to the adverse effects of steric shielding and carbohydrate ligand accessibility.

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http://dx.doi.org/10.1021/acs.biomac.0c00676DOI Listing

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