Biochemical Mechanism of Hepatitis C Virus Inhibition by the Broad-Spectrum Antiviral Arbidol

Pécheur, Eve Isabelle; Lavillette, Dimitri; Alcaras, Fanny; Molle, Jennifer; Boriskin, Yu. S.; Roberts, Margaret; Cosset, François‐Loïc; Polyak, Stephen J.

doi:10.1021/bi700181j

Cited by 76 publications

(114 citation statements)

References 45 publications

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“…2A indicate that arbidol can efficiently inhibit Jc1 virus membrane fusion, in a dose-dependent manner. The concentration of arbidol able to inhibit fusion by 50% (IC 50 ) was ϳ2 g/ml, in close agreement with our previous data on HCVpp (53,54). When the virus was preincubated with arbidol before infection of Huh-7.5 cells and inoculation was done in the presence of the drug, a dose-dependent reduction of infectivity was observed, with a 50% inhibition at ϳ6 g/ml arbidol (Fig.…”

Section: Resultssupporting

confidence: 90%

“…This is the first direct description of HCV fusion characteristics in a genotype 2a context using physio-pathologically relevant HCVcc particles. Moreover, assessing the interference of arbidol, a small fusion inhibitor molecule recently described by us as a potential HCV entry inhibitor (52)(53)(54), further confirmed the utility of the HCVcc fusion assay for the characterization of HCV fusion inhibitors (Fig. 2).…”

Section: Discussionsupporting

confidence: 59%

“…We recently described an anti-HCV activity of arbidol that is based on inhibition of HCV cell entry and membrane fusion by the drug (53,54). However, in our previous work the fusion inhibition exerted by arbidol was only assessed using HCV pseudoparticles.…”

Section: Resultsmentioning

confidence: 99%

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Low pH-dependent Hepatitis C Virus Membrane Fusion Depends on E2 Integrity, Target Lipid Composition, and Density of Virus Particles

Haid

Pietschmann

Pécheur

2009

Journal of Biological Chemistry

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Hepatitis C virus (HCV) is an enveloped, positive strand RNA virus of about 9.6 kb. Like all enveloped viruses, the HCV membrane fuses with the host cell membrane during the entry process and thereby releases the genome into the cytoplasm, initiating the viral replication cycle. To investigate the features of HCV membrane fusion, we developed an in vitro fusion assay using cell culture-produced HCV and fluorescently labeled liposomes. With this model we could show that HCV-mediated fusion can be triggered in a receptor-independent but pH-dependent manner and that fusion of the HCV particles with liposomes is dependent on the viral dose and on the lipid composition of the target membranes. In addition CBH-5, an HCV E2-specific antibody, inhibited fusion in a dose-dependent manner. Interestingly, point mutations in E2, known to abrogate HCV glycoprotein-mediated fusion in a cell-based assay, altered or even abolished fusion in the liposome-based assay. When assaying the fusion properties of HCV particles with different buoyant density, we noted higher fusogenicity of particles with lower density. This could be attributable to inherently different properties of low density particles, to association of these particles with factors stimulating fusion, or to co-floatation of factors enhancing fusion activity in trans. Taken together, these data show the important role of lipids of both the viral and target membranes in HCV-mediated fusion, point to a crucial role played by the E2 glycoprotein in the process of HCV fusion, and reveal an important behavior of HCV of different densities with regard to fusion. Hepatitis C virus (HCV)4 is an important public health concern worldwide as it is a major cause of chronic hepatitis, cirrhosis, and hepatocellular carcinoma. HCV is an enveloped virus that belongs to the Hepacivirus genus of the Flaviviridae family (1). Based on sequence comparison, patient isolates are classified into seven genotypes, differing in their nucleotide sequence by 30 -35% (2-5). The two viral surface proteins, E1 (residues 192-383) and E2 (residues 384 -746), are processed by signal peptidases of the endoplasmic reticulum from a 3,000-amino acid-long polyprotein encoded by the HCV genome (reviewed in Ref.2). The E1 (ϳ31 kDa) and E2 (ϳ70 kDa) proteins are glycosylated in their large amino-terminal ectodomains (6) and are anchored in the viral membrane by their carboxyl-terminal transmembrane domains. E1 and E2 form a heterodimer stabilized by noncovalent interactions. This oligomer is thought to be present at the surface of HCV particles (7) and to be involved in viral entry. Carboxyl-terminally truncated soluble E2 protein is known to specifically bind to crucial HCV entry factors like glycosaminoglycans, the tetraspanin CD81, and the scavenger receptor BI (8 -12). Thus, virus-associated E2 is likely directly involved in interactions important for virus attachment and productive infection (reviewed in Refs. 13,14).Both HCV envelope glycoproteins are the targets for virusneutralizing antibodies (7,(15)...

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Section: Resultssupporting

confidence: 90%

Section: Discussionsupporting

confidence: 59%

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Low pH-dependent Hepatitis C Virus Membrane Fusion Depends on E2 Integrity, Target Lipid Composition, and Density of Virus Particles

Haid

Pietschmann

Pécheur

2009

Journal of Biological Chemistry

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“…Anti-E1/E2 Abs [9,11,62,148], patient sera [9], soluble E2 [46], lectins [150,151], anti-ApoE antibodies [29], apoE peptides [149] Abs, Erlotinib, Lapatinib, Gefitinib [141] EGF, TGF-α [141] HDL [138] ApoCI [139] BLTs [138,140] Abs, Dasatinib [141] Arbidol [144] Abs [109,137], ITX 5061 [134], natural ligands [135,136] Abs, soluble CD81 [9,11] Abs [142] Cldn1 peptide [143] Heparin, GAG nzymatic digestion [69,132] Abs, natural ligands, soluble LDL receptor [30,133] GAGs LDLR CD81 SR-BI Cldn1 Ocln…”

Section: Epha2mentioning

confidence: 99%

Section: Epha2mentioning

confidence: 99%

Entry and replication of recombinant hepatitis C viruses in cell culture

Vièyres

Pietschmann

2013

Methods

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Pd‐Catalyzed MIA‐Directed Acetoxylation of Benzylamines and Computational Study

et al. 2022

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The direct acetoxylation of substituted benzylamines has been accomplished through methoxyiminoacyl (MIA)‐mediated Pd‐catalyzed C−H functionalization. A diverse array of phenylalanine substrates is amenable to this protocol, providing acetoxylation benzylamine derivatives with good to high efficiency. Computational results revealed that HOAc enhanced the stability of Pd−O bond, which obviously accelerate the reductive elimination step of the acetoxylation process.

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Biochemical Mechanism of Hepatitis C Virus Inhibition by the Broad-Spectrum Antiviral Arbidol

Cited by 76 publications

References 45 publications

Low pH-dependent Hepatitis C Virus Membrane Fusion Depends on E2 Integrity, Target Lipid Composition, and Density of Virus Particles

Low pH-dependent Hepatitis C Virus Membrane Fusion Depends on E2 Integrity, Target Lipid Composition, and Density of Virus Particles

Entry and replication of recombinant hepatitis C viruses in cell culture

Pd‐Catalyzed MIA‐Directed Acetoxylation of Benzylamines and Computational Study

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