Characterization of the hepatitis C virus E2 epitope defined by the broadly neutralizing monoclonal antibody AP33

Tarr, Alexander W.; Owsianka, Ania M.; Timms, Judith; McClure, C. Patrick; Brown, Richard J. P.; Hickling, Timothy P.; Pietschmann, Thomas; Bartenschlager, Ralf; Patel, Arvind H.; Ball, Jonathan K.

doi:10.1002/hep.21088

Cited by 142 publications

(193 citation statements)

References 47 publications

Supporting

Mentioning

176

Contrasting

Order By: Relevance

“…Similarly, W420A mutation abolished both MAb AP33 (itself a broadly neutralizing antibody [39]) and CD81 binding, indicating overlap between the CD81 binding site and the AP33 epitope. Finally, mutations at L413, N415, and G418 also reduced the binding of MAb AP33, and we have recently shown that these, together with W420, are probable contact residues (47).…”

Section: Discussionmentioning

confidence: 71%

See 1 more Smart Citation

Identification of Conserved Residues in the E2 Envelope Glycoprotein of the Hepatitis C Virus That Are Critical for CD81 Binding

Owsianka

Timms

Tarr

et al. 2006

J Virol

Self Cite

228

268

View full text Add to dashboard Cite

Hepatitis C virus (HCV) cell entry involves interaction between the viral envelope glycoprotein E2 and the cell surface receptor CD81. Knowledge of conserved E2 determinants important for successful binding will facilitate development of entry inhibitors designed to block this interaction. Previous studies have assigned the CD81 binding function to a number of discontinuous regions of E2. To better define specific residues involved in receptor binding, a panel of mutants of HCV envelope proteins was generated, where conserved residues within putative CD81 binding regions were sequentially mutated to alanine. Mutant proteins were tested for binding to a panel of monoclonal antibodies and CD81 and for their ability to form noncovalent heterodimers and confer infectivity in the retroviral pseudoparticle (HCVpp) assay. Detection by conformation-sensitive monoclonal antibodies indicated that the mutant proteins were correctly folded. Mutant proteins fell into three groups: those that bound CD81 and conferred HCVpp infectivity, those that abrogated both CD81 binding and HCVpp infectivity, and a final group containing mutants that were able to bind CD81 but were noninfectious in the HCVpp assay. Specific amino acids conserved across all genotypes that were critical for CD81 binding were W420, Y527, W529, G530, and D535. These data significantly increase our understanding of the CD81 receptor-E2 binding process.Hepatitis C virus (HCV) is the sole member of the Hepacivirus genus within the family Flaviviridae. It is a major cause of community-acquired and posttransfusion hepatitis. More than 170 million people worldwide are seropositive for HCV, and only 20% of those infected are able to clear the virus. In the remaining 80% of individuals, the virus persists and can

show abstract

Section: Discussionmentioning

confidence: 71%

“…The majority of the substitutions were tolerated by MAb AP33, although binding to mutants L413A, N415A, G418A, and W420A was reduced by at least 50% compared to the wild-type protein. We have recently shown that these residues form part of the AP33 epitope (47). Recognition of the mutant proteins by three conformation-depen-FIG.…”

Section: Resultsmentioning

confidence: 99%

Identification of Conserved Residues in the E2 Envelope Glycoprotein of the Hepatitis C Virus That Are Critical for CD81 Binding

Owsianka

Timms

Tarr

et al. 2006

J Virol

Self Cite

228

268

View full text Add to dashboard Cite

show abstract

“…These mutations were not found in virus passaged in parallel without AP33 neutralization. Although N415 is within a domain identified previously as comprising the AP33 epitope 413-420 (22,23), E655 is distant in the linear E2 sequence and has not been implicated previously in recognition of HCV by AP33. To validate the role of these mutations in conferring neutralization escape, they were engineered both singly and together into pHJ3-5 plasmid DNA, and the cognate viruses rescued after RNA transfection of naive cells.…”

Section: Resultsmentioning

confidence: 89%

“…Importantly, immunization of mice and rats with recombinant E2 also elicits mAbs that recognize this E2 segment (20)(21)(22). One such mAb, AP33, is of particular interest because it demonstrates broad and potent, cross-genotypic neutralizing activity.…”

mentioning

confidence: 99%

“…One such mAb, AP33, is of particular interest because it demonstrates broad and potent, cross-genotypic neutralizing activity. Prior studies using synthetic peptides, recombinant antigens, and HCVpp suggest that AP33 binds a highly conserved, linear epitope spanning residues 413-420 (22,23). Here, we describe the use of a cell culture-infectious, intergenotypic chimeric HCV with genotype 1a structural proteins (24,25) to further define the AP33 epitope by analyzing mutants selected for the ability to escape neutralization by this mAb.…”

mentioning

confidence: 99%

See 1 more Smart Citation

In vitro selection of a neutralization-resistant hepatitis C virus escape mutant

Gal-Tanamy

Keck

et al. 2008

Proc. Natl. Acad. Sci. U.S.A.

Self Cite

View full text Add to dashboard Cite

Effective immunization against hepatitis C virus (HCV) infections is likely to require the induction of both robust T and B cell immunity. Although neutralizing antibodies may play an important role in control of infection, there is little understanding of the structure of the HCV envelope glycoproteins and how they interact with such antibodies. An additional challenge for vaccine design is the genetic diversity of HCV and the rapid evolution of viral quasispecies that escape antibody-mediated neutralization. We used a cell culture-infectious, chimeric HCV with the structural proteins of genotype 1a virus to identify envelope residues contributing to the epitope recognized by a broadly neutralizing, murine monoclonal antibody, AP33. By repetitive rounds of neutralization followed by amplification, we selected a population of viral escape mutants that resist stringent neutralization with AP33 and no longer bind the antibody. Two amino acid substitutions, widely separated in the linear sequence of the E2 envelope protein (N415Y and E655G), were identified by sequencing of cloned cDNA and shown by reverse genetics analysis to contribute jointly to the AP33 resistance phenotype. The N415Y mutation substantially lowered virus fitness, most likely because of a defect in viral entry, but did not reduce binding of soluble CD81 to immobilized HCV-pseudotyped retrovirus particles. The in vitro selection of an HCV escape mutant recapitulates the ongoing evolution of antigenic variants that contributes to viral persistence in humans and reveals information concerning the conformational structure of the AP33 epitope, its role in viral replication, and constraints on its molecular evolution.antibody ͉ immunity ͉ vaccine ͉ viral envelope

show abstract

Viral Escape Mechanisms in Hepatitis C and the Clinical Consequences of Persistent Infection

Lemon¹,

Farci

Ghany

2009

The Liver

View full text Add to dashboard Cite

Characterization of the hepatitis C virus E2 epitope defined by the broadly neutralizing monoclonal antibody AP33

Cited by 142 publications

References 47 publications

Identification of Conserved Residues in the E2 Envelope Glycoprotein of the Hepatitis C Virus That Are Critical for CD81 Binding

Identification of Conserved Residues in the E2 Envelope Glycoprotein of the Hepatitis C Virus That Are Critical for CD81 Binding

In vitro selection of a neutralization-resistant hepatitis C virus escape mutant

Viral Escape Mechanisms in Hepatitis C and the Clinical Consequences of Persistent Infection

Contact Info

Product

Resources

About