Inhibition of Influenza Virus Activity by Multivalent Glycoarchitectures with Matched Sizes

被引:94
作者
Papp, Ilona [1 ]
Sieben, Christian [2 ]
Sisson, Adam L. [3 ,4 ]
Kostka, Johanna [2 ]
Boettcher, Christoph [5 ]
Ludwig, Kai [5 ]
Herrmann, Andreas [2 ]
Haag, Rainer [1 ]
机构
[1] Free Univ Berlin, Inst Chem & Biochem, D-14195 Berlin, Germany
[2] Humboldt Univ, Inst Biol Mol Biophys, D-10115 Berlin, Germany
[3] HZG Forschungszentrum Geesthacht GmbH, Ctr Biomat Dev, Polymer Res Inst, D-14513 Teltow, Germany
[4] HZG Forschungszentrum Geesthacht GmbH, Berlin Brandenburg Ctr Regenerat Therapies BCRT, Polymer Res Inst, D-14513 Teltow, Germany
[5] Free Univ Berlin, Inst Chem & Biochem, Forschungszentrum Elektronenmikroskopie, D-14195 Berlin, Germany
关键词
influenza; multivalent inhibition; nanogels; polyglycerol; sialic acids; viruses; CLUSTER SIALOSIDE INHIBITORS; SOLID-PHASE SYNTHESIS; SIALIC-ACID; CHEMOENZYMATIC SYNTHESIS; CATIONIC-POLYMERIZATION; POTENT INHIBITORS; A VIRUS; BINDING; HEMAGGLUTINATION; AGGLUTINATION;
D O I
10.1002/cbic.201000776
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
We describe the synthesis of a series of sialic acid-conjugated, polyglycerol-based nanoparticles with diameters in the range of 1-100 nm. Particle sizes were varied along with the degree of functionalization to match the corresponding virus size and receptor multiplicity in order to achieve maximum efficiency. To build up these architectures, we used biocompatible, hyperbranched polyglycerols as scaffolds and recently developed polyglycerol-based nanogels, the sizes of which can be varied between 2-4 nm and 40-100 nm, respectively. We demonstrate here that such multivalent nanoparticles inhibit influenza A virus cell binding and fusion and consequently infectivity. The potential of multivalency is evident from larger particles showing very efficient inhibition of viral infection up to 80%. Indeed, both the size of the nanoparticle and the amount of ligand density are important determinants of inhibition efficiency. The inhibitory activity of the tested polymeric nanoparticles drastically increased with size. Particles with similar dimensions to the virus (50-100 nm) are exceedingly effective. We also observed a saturation point in degree of surface functionalization (i.e. ligand density), above which inhibition was not significantly improved. Our study emphasizes the importance of matching particle sizes and ligand densities to mimic biological surfaces and improve interactions; this is a vital concept underlying multivalent interactions.
引用
收藏
页码:887 / 895
页数:9
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