Full-Length Characterization of Hepatitis C Virus Subtype 3a Reveals Novel Hypervariable Regions under Positive Selection during Acute Infection
Full-Length Characterization of Hepatitis C Virus Subtype 3a Reveals Novel Hypervariable Regions under Positive Selection during Acute Infection
Hepatitis C virus subtype 3a is a highly prevalent and globally distributed strain that is often associated with infection via injection drug use. This subtype exhibits particular phenotypic characteristics. In spite of this, detailed genetic analysis of this subtype has rarely been performed. We performed full-length viral sequence analysis in 18 patients with chronic HCV subtype 3a infection and assessed genomic viral variability in comparison to other HCV subtypes. Two novel regions of intragenotypic hypervariability within the envelope protein E2, of HCV genotype 3a, were identified. We named these regions HVR495 and HVR575. They consisted of flanking conserved hydrophobic amino acids and central variable residues. A 5-amino-acid insertion found only in genotype 3a and a putative glycosylation site is contained within HVR575. Evolutionary analysis of E2 showed that positively selected sites within genotype 3a infection were largely restricted to HVR1, HVR495, and HVR575. Further analysis of clonal viral populations within single hosts showed that viral variation within HVR495 and HVR575 were subject to intrahost positive selecting forces. Longitudinal analysis of four patients with acute HCV subtype 3a infection sampled at multiple time points showed that positively selected mutations within HVR495 and HVR575 arose early during primary infection. HVR495 and HVR575 were not present in HCV subtypes 1a, 1b, 2a, or 6a. Some variability that was not subject to positive selection was present in subtype 4a HVR575. Further defining the functional significance of these regions may have important implications for genotype 3a E2 virus-receptor interactions and for vaccine studies that aim to induce cross-reactive anti-E2 antibodies.
11456 - 11466
Humphreys, Isla
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Fleming, Vicki
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Fabris, Paolo
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Parker, Joe
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Schulenberg, Bodo
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Brown, Anthony
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Demetriou, Charis
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Gaudieri, Silvana
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Pfafferott, Katja
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Lucas, Michaela
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Collier, Jane
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Huang, Kuan-Hsiang Gary
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Pybus, Oliver G.
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Klenerman, Paul
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Barnes, Eleanor
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November 2009
Humphreys, Isla
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Fleming, Vicki
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Fabris, Paolo
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Parker, Joe
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Schulenberg, Bodo
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Brown, Anthony
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Demetriou, Charis
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Gaudieri, Silvana
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Pfafferott, Katja
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Lucas, Michaela
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Collier, Jane
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Huang, Kuan-Hsiang Gary
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Pybus, Oliver G.
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Klenerman, Paul
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Barnes, Eleanor
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Humphreys, Isla, Fleming, Vicki, Fabris, Paolo, Parker, Joe, Schulenberg, Bodo, Brown, Anthony, Demetriou, Charis, Gaudieri, Silvana, Pfafferott, Katja, Lucas, Michaela, Collier, Jane, Huang, Kuan-Hsiang Gary, Pybus, Oliver G., Klenerman, Paul and Barnes, Eleanor
(2009)
Full-Length Characterization of Hepatitis C Virus Subtype 3a Reveals Novel Hypervariable Regions under Positive Selection during Acute Infection.
Journal of Virology, 83 (22), .
(doi:10.1128/jvi.00884-09).
Abstract
Hepatitis C virus subtype 3a is a highly prevalent and globally distributed strain that is often associated with infection via injection drug use. This subtype exhibits particular phenotypic characteristics. In spite of this, detailed genetic analysis of this subtype has rarely been performed. We performed full-length viral sequence analysis in 18 patients with chronic HCV subtype 3a infection and assessed genomic viral variability in comparison to other HCV subtypes. Two novel regions of intragenotypic hypervariability within the envelope protein E2, of HCV genotype 3a, were identified. We named these regions HVR495 and HVR575. They consisted of flanking conserved hydrophobic amino acids and central variable residues. A 5-amino-acid insertion found only in genotype 3a and a putative glycosylation site is contained within HVR575. Evolutionary analysis of E2 showed that positively selected sites within genotype 3a infection were largely restricted to HVR1, HVR495, and HVR575. Further analysis of clonal viral populations within single hosts showed that viral variation within HVR495 and HVR575 were subject to intrahost positive selecting forces. Longitudinal analysis of four patients with acute HCV subtype 3a infection sampled at multiple time points showed that positively selected mutations within HVR495 and HVR575 arose early during primary infection. HVR495 and HVR575 were not present in HCV subtypes 1a, 1b, 2a, or 6a. Some variability that was not subject to positive selection was present in subtype 4a HVR575. Further defining the functional significance of these regions may have important implications for genotype 3a E2 virus-receptor interactions and for vaccine studies that aim to induce cross-reactive anti-E2 antibodies.
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Published date: November 2009
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Local EPrints ID: 480463
URI: http://eprints.soton.ac.uk/id/eprint/480463
ISSN: 0022-538X
PURE UUID: 5a04bd5d-1317-48b4-b678-0406965edd63
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Date deposited: 02 Aug 2023 17:09
Last modified: 18 Mar 2024 03:50
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Contributors
Author:
Isla Humphreys
Author:
Vicki Fleming
Author:
Paolo Fabris
Author:
Bodo Schulenberg
Author:
Anthony Brown
Author:
Charis Demetriou
Author:
Silvana Gaudieri
Author:
Katja Pfafferott
Author:
Michaela Lucas
Author:
Jane Collier
Author:
Kuan-Hsiang Gary Huang
Author:
Oliver G. Pybus
Author:
Paul Klenerman
Author:
Eleanor Barnes
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