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Exploring Rigid and Flexible Core Trivalent Sialosides for Influenza Virus Inhibition.


ABSTRACT: Herein, the chemical synthesis and binding analysis of functionalizable rigid and flexible core trivalent sialosides bearing oligoethylene glycol (OEG) spacers interacting with spike proteins of influenza?A virus (IAV) X31 is described. Although the flexible Tris-based trivalent sialosides achieved micromolar binding constants, a trivalent binder based on a rigid adamantane core dominated flexible tripodal compounds with micromolar binding and hemagglutination inhibition constants. Simulation studies indicated increased conformational penalties for long OEG spacers. Using a systematic approach with molecular modeling and simulations as well as biophysical analysis, these findings emphasize on the importance of the scaffold rigidity and the challenges associated with the spacer length optimization.

SUBMITTER: Kiran P 

PROVIDER: S-EPMC6587447 | biostudies-literature | 2018 Dec

REPOSITORIES: biostudies-literature

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Exploring Rigid and Flexible Core Trivalent Sialosides for Influenza Virus Inhibition.

Kiran Pallavi P   Bhatia Sumati S   Lauster Daniel D   Aleksić Stevan S   Fleck Carsten C   Peric Natalija N   Maison Wolfgang W   Liese Susanne S   Keller Bettina G BG   Herrmann Andreas A   Haag Rainer R  

Chemistry (Weinheim an der Bergstrasse, Germany) 20181122 72


Herein, the chemical synthesis and binding analysis of functionalizable rigid and flexible core trivalent sialosides bearing oligoethylene glycol (OEG) spacers interacting with spike proteins of influenza A virus (IAV) X31 is described. Although the flexible Tris-based trivalent sialosides achieved micromolar binding constants, a trivalent binder based on a rigid adamantane core dominated flexible tripodal compounds with micromolar binding and hemagglutination inhibition constants. Simulation st  ...[more]

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