Literature DB >> 23362274

Sialylneolacto-N-tetraose c (LSTc)-bearing liposomal decoys capture influenza A virus.

Gabriel L Hendricks1, Kim L Weirich, Karthik Viswanathan, Jing Li, Zachary H Shriver, Joseph Ashour, Hidde L Ploegh, Evelyn A Kurt-Jones, Deborah K Fygenson, Robert W Finberg, James C Comolli, Jennifer P Wang.   

Abstract

Influenza is a severe disease in humans and animals with few effective therapies available. All strains of influenza virus are prone to developing drug resistance due to the high mutation rate in the viral genome. A therapeutic agent that targets a highly conserved region of the virus could bypass resistance and also be effective against multiple strains of influenza. Influenza uses many individually weak ligand binding interactions for a high avidity multivalent attachment to sialic acid-bearing cells. Polymerized sialic acid analogs can form multivalent interactions with influenza but are not ideal therapeutics due to solubility and toxicity issues. We used liposomes as a novel means for delivery of the glycan sialylneolacto-N-tetraose c (LSTc). LSTc-bearing decoy liposomes form multivalent, polymer-like interactions with influenza virus. Decoy liposomes competitively bind influenza virus in hemagglutination inhibition assays and inhibit infection of target cells in a dose-dependent manner. Inhibition is specific for influenza virus, as inhibition of Sendai virus and respiratory syncytial virus is not observed. In contrast, monovalent LSTc does not bind influenza virus or inhibit infectivity. LSTc decoy liposomes prevent the spread of influenza virus during multiple rounds of replication in vitro and extend survival of mice challenged with a lethal dose of virus. LSTc decoy liposomes co-localize with fluorescently tagged influenza virus, whereas control liposomes do not. Considering the conservation of the hemagglutinin binding pocket and the ability of decoy liposomes to form high avidity interactions with influenza hemagglutinin, our decoy liposomes have potential as a new therapeutic agent against emerging influenza strains.

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Year:  2013        PMID: 23362274      PMCID: PMC3605625          DOI: 10.1074/jbc.M112.437202

Source DB:  PubMed          Journal:  J Biol Chem        ISSN: 0021-9258            Impact factor:   5.157


  43 in total

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Authors:  Y Ha; D J Stevens; J J Skehel; D C Wiley
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Authors:  S A Feldman; S Audet; J A Beeler
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Authors:  Chao-Tan Guo; Xue-Long Sun; Osamu Kanie; Kennedy Francis Shortridge; Takashi Suzuki; Daisei Miyamoto; Kazuya I-P Jwa Hidari; Chi-Huey Wong; Yasuo Suzuki
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Authors:  M A Markwell; J C Paulson
Journal:  Proc Natl Acad Sci U S A       Date:  1980-10       Impact factor: 11.205

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Authors:  T J Pritchett; R Brossmer; U Rose; J C Paulson
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Authors:  Jennifer E Stencel-Baerenwald; Kerstin Reiss; Dirk M Reiter; Thilo Stehle; Terence S Dermody
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Authors:  Lavanya Singh; Hendrik G Kruger; Glenn E M Maguire; Thavendran Govender; Raveen Parboosing
Journal:  Ther Adv Infect Dis       Date:  2017-07-05

3.  Nanostructured glycan architecture is important in the inhibition of influenza A virus infection.

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8.  Multivalent Peptide-Nanoparticle Conjugates for Influenza-Virus Inhibition.

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Review 9.  SARS-CoV-2 and its new variants: a comprehensive review on nanotechnological application insights into potential approaches.

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Review 10.  New small-molecule drug design strategies for fighting resistant influenza A.

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Journal:  Acta Pharm Sin B       Date:  2015-09-06       Impact factor: 11.413

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