Effect of Hemagglutinin Glycosylation on Influenza Virus Susceptibility to Neuraminidase Inhibitors

Mishin, Vasiliy P.; Novikov, D V; Hayden, Frederick G.; Gubareva, Larisa V.

doi:10.1128/jvi.79.19.12416-12424.2005

Cited by 55 publications

(50 citation statements)

References 55 publications

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“…By using different biochemical approaches, we show that TIZ blocks HA terminal glycosylation at a stage preceding resistance to endoglycosidase H digestion, which is a marker for transport into the cis and middle Golgi compartments (29). Immunomicroscopy studies and analysis of viral particles produced by infected cells confirm that the TIZ-induced alterations impair HA0 trafficking between the endoplasmic reticulum and the Golgi complex, preventing its transport and insertion into the host cell plasma membrane and blocking the exit of mature virions from host cells.…”

Section: Discussionmentioning

confidence: 99%

“…The mannose-rich sugar component is processed in the Golgi apparatus during the transport to the cell surface, and terminal glycosylation occurs in trans cisternae of the Golgi apparatus (27). To investigate whether TIZ could affect HA0 passage through the Golgi, we subjected aliquots of radiolabeled proteins and HA0 immunoprecipitated samples to digestion with Endo-H, an enzyme that removes N-linked carbohydrate chains that have not been terminally glycosylated (28) or with PNGase-F, an enzyme that removes all N-glycans (29). As expected, both forms of the protein were sensitive to PNGase-F digestion; however, whereas HA0 from control cells was terminally glysosylated becoming Endo-H-resistant, HA0 from TIZ-treated cells remained sensitive to digestion with the protease up to 4 h after synthesis (Fig.…”

Section: Antiviral Activity Of Thiazolides Against Differentmentioning

confidence: 99%

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Thiazolides, a New Class of Anti-influenza Molecules Targeting Viral Hemagglutinin at the Post-translational Level

Rossignol

Frazia

Chiappa

et al. 2009

Journal of Biological Chemistry

224

253

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The emergence of highly contagious influenza A virus strains, such as the new H1N1 swine influenza, represents a serious threat to global human health. Efforts to control emerging influenza strains focus on surveillance and early diagnosis, as well as development of effective vaccines and novel antiviral drugs. Herein we document the anti-influenza activity of the anti-infective drug nitazoxanide and its active circulating-metabolite tizoxanide and describe a class of second generation thiazolides effective against influenza A virus. Thiazolides inhibit the replication of H1N1 and different other strains of influenza A virus by a novel mechanism: they act at post-translational level by selectively blocking the maturation of the viral hemagglutinin at a stage preceding resistance to endoglycosidase H digestion, thus impairing hemagglutinin intracellular trafficking and insertion into the host plasma membrane, a key step for correct assembly and exit of the virus from the host cell. Targeting the maturation of the viral glycoprotein offers the opportunity to disrupt the production of infectious viral particles attacking the pathogen at a level different from the currently available anti-influenza drugs. The results indicate that thiazolides may represent a new class of antiviral drugs effective against influenza A infection.

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Section: Discussionmentioning

confidence: 99%

Section: Antiviral Activity Of Thiazolides Against Differentmentioning

confidence: 99%

Thiazolides, a New Class of Anti-influenza Molecules Targeting Viral Hemagglutinin at the Post-translational Level

Rossignol

Frazia

Chiappa

et al. 2009

Journal of Biological Chemistry

224

253

View full text Add to dashboard Cite

show abstract

“…Based on the ability of EB to inhibit viral attachment, we hypothesized that the peptide interacted with either NA or HA since changes to either surface glycoprotein can alter fitness of the virus (22). To determine if EB inhibited NA enzymatic activity, untreated or peptide-treated Tk/Ont was tested for enzymatic activity by MUNANA [2Ј-(4-methylumbelliferyl)-␣-D-N-acetylneuraminic acid].…”

Section: Efficacy In Vivomentioning

confidence: 99%

Inhibition of Influenza Virus Infection by a Novel Antiviral Peptide That Targets Viral Attachment to Cells

Jones¹,

Turpin²,

Bultmann

et al. 2006

J Virol

148

147

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Influenza A viruses continue to cause widespread morbidity and mortality. There is an added concern that the highly pathogenic H5N1 influenza A viruses, currently found throughout many parts of the world, represent a serious public health threat and may result in a pandemic. Intervention strategies to halt an influenza epidemic or pandemic are a high priority, with an emphasis on vaccines and antiviral drugs. In these studies, we demonstrate that a 20-amino-acid peptide (EB, for entry blocker) derived from the signal sequence of fibroblast growth factor 4 exhibits broad-spectrum antiviral activity against influenza viruses including the H5N1 subtype in vitro. The EB peptide was protective in vivo, even when administered postinfection. Mechanistically, the EB peptide inhibits the attachment to the cellular receptor, preventing infection. Further studies demonstrated that the EB peptide specifically binds to the viral hemagglutinin protein. This novel peptide has potential value as a reagent to study virus attachment and as a future therapeutic.

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“…Although glycosylation sites were not necessary for the survival of influenza virus, they played an important role in determining some properties of these viruses. Vasiliy [ see 27,28] reported that a negatively charged glycosylation site near HA RB sites affect HA receptor binding, leading to reduced influenza virus dependence on NA which was the target of antiinfluenza drug failure. Furthermore, the 3 RB sites underwent considerable changes with time.…”

Section: Discussionmentioning

confidence: 99%

Evolutionary Characterization of Human H1N1 Influenza Virus Hemagglutinin Genes Isolated from 1947 to 2009 in China

Liu

Zhang²,

Wang³

et al. 2011

Intervirology

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Objective: Our aim was to reveal the molecular characteristics of human H1N1 influenza virus hemagglutinin (HA) genes from 1947 to 2009 in China. Methods: 129 HA gene sequences were downloaded from NCBI’s GenBank and analyzed by DNASTAR software. Additionally, the three-dimensional structure of HA protein was predicted by the SWISS-MODEL service. Results: First, 2009 Chinese HA genes were 99% identical to those of Mexican and American ones; their key sites remained highly conserved. Second, 50 Chinese strains from 1947 to 2009 clustered by the year of isolation, and 2009 strains had only 70% identity to 1947–2008 ones. Third, over the past 60 years, 3 receptor-binding (RB) sites and 2 of the 8 glycosylation sites (amino acids 279 and 290) underwent considerable changes while the cleavage sites remained stable. Fourth, the human HA sequences differed completely from swine and avian isolates. Finally, the mutation of cleavage sites can change the three-dimensional structures, but single mutations cannot. Conclusions: Thus, in the past 60 years, Chinese H1N1 influenza HA genes kept stable with high affinity and low pathogenicity to human except changes in 2 glycosylation and 3 RB sites which were associated with the pandemic strength, range and host specificity of viruses.

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Effect of Hemagglutinin Glycosylation on Influenza Virus Susceptibility to Neuraminidase Inhibitors

Cited by 55 publications

References 55 publications

Thiazolides, a New Class of Anti-influenza Molecules Targeting Viral Hemagglutinin at the Post-translational Level

Thiazolides, a New Class of Anti-influenza Molecules Targeting Viral Hemagglutinin at the Post-translational Level

Inhibition of Influenza Virus Infection by a Novel Antiviral Peptide That Targets Viral Attachment to Cells

Evolutionary Characterization of Human H1N1 Influenza Virus Hemagglutinin Genes Isolated from 1947 to 2009 in China

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