Linear Polysialoside Outperforms Dendritic Analogs for Inhibition of Influenza Virus Infection In vitro and In vivo

Overview

Journal Biomaterials

Specialty Biomedical Engineering

Date 2017 May 28

PMID 28550754

Citations 29

Authors

Sumati Bhatia

Daniel Lauster

Markus Bardua

Kai Ludwig

Stefano Angioletti-Uberti

Nicole Popp

Ute Hoffmann

Florian Paulus

Matthias Budt

Marlena Stadtmuller

Thorsten Wolff

Alf Hamann

Christoph Bottcher

Andreas Herrmann

Rainer Haag

Affiliations

Soon will be listed here.

Abstract

Inhibition of influenza A virus infection by multivalent sialic acid inhibitors preventing viral hemagglutinin binding to host cells of the respiratory tract is a promising strategy. However, optimal geometry and optimal ligand presentation on multivalent scaffolds for efficient inhibition both in vitro and in vivo application are still unclear. Here, by comparing linear and dendritic polyglycerol sialosides (LPGSA and dPGSA) we identified architectural requirements and optimal ligand densities for an efficient multivalent inhibitor of influenza virus A/X31/1 (H3N2). Due to its large volume, the LPGSA at optimal ligand density sterically shielded the virus significantly better than the dendritic analog. A statistical mechanics model rationalizes the relevance of ligand density, morphology, and the size of multivalent scaffolds for the potential to inhibit virus-cell binding. Optimized LPGSA inhibited virus infection at IC in the low nanomolar nanoparticle concentration range and also showed potent antiviral activity against two avian influenza strains A/Mallard/439/2004 (H3N2) and A/turkey/Italy/472/1999 (H7N1) post infection. In vivo application of inhibitors clearly confirmed the higher inhibition potential of linear multivalent scaffolds to prevent infection. The optimized LPGSA did not show any acute toxicity, and was much more potent than the neuraminidase inhibitor oseltamivir carboxylate in vivo. Combined application of the LPGSA and oseltamivir carboxylate revealed a synergistic inhibitory effect and successfully prevented influenza virus infection in mice.

Citing Articles

Branched Polymer Architecture for Modulating Interactions in Material-Bio Interface.

Taghavimandi F, Kim M, Lee M, Shin K Tissue Eng Regen Med. 2025; .

PMID: 40056364 DOI: 10.1007/s13770-024-00699-1.

Quantitative Prediction of Protein-Polyelectrolyte Binding Thermodynamics: Adsorption of Heparin-Analog Polysulfates to the SARS-CoV-2 Spike Protein RBD.

Neander L, Hannemann C, Netz R, Sahoo A JACS Au. 2025; 5(1):204-216.

PMID: 39886596 PMC: 11775700. DOI: 10.1021/jacsau.4c00886.

Lignin-Based Mucus-Mimicking Antiviral Hydrogels with Enzyme Stability and Tunable Porosity.

Chandna S, Povolotsky T, Nie C, Schwartz S, Wedepohl S, Quaas E ACS Appl Mater Interfaces. 2025; 17(6):8962-8975.

PMID: 39876589 PMC: 11826508. DOI: 10.1021/acsami.4c18519.

Sulfated Cellulose Nanofiber Hydrogel with Mucus-Like Activities for Virus Inhibition.

Long Y, Dimde M, Adler J, Vidal R, Povolotsky T, Nickl P ACS Appl Mater Interfaces. 2024; 16(49):67504-67513.

PMID: 39582136 PMC: 11647751. DOI: 10.1021/acsami.4c17998.

Drug resistance and possible therapeutic options against influenza A virus infection over past years.

Asif Raza M, Ashraf M Arch Microbiol. 2024; 206(12):458.

PMID: 39499323 DOI: 10.1007/s00203-024-04181-3.