Literature DB >> 9573256

Long-term evolution of the hypervariable region of hepatitis C virus in a common-source-infected cohort.

J McAllister1, C Casino, F Davidson, J Power, E Lawlor, P L Yap, P Simmonds, D B Smith.   

Abstract

The long-term evolution of the hepatitis C virus hypervariable region (HVR) and flanking regions of the E1 and E2 envelope proteins have been studied in a cohort of women infected from a common source of anti-D immunoglobulin. Whereas virus sequences in the infectious source were relatively homogeneous, distinct HVR variants were observed in each anti-D recipient, indicating that this region can evolve in multiple directions from the same point. Where HVR variants with dissimilar sequences were present in a single individual, the frequency of synonymous substitution in the flanking regions suggested that the lineages diverged more than a decade previously. Even where a single major HVR variant was present in an infected individual, this lineage was usually several years old. Multiple lineages can therefore coexist during long periods of chronic infection without replacement. The characteristics of amino acid substitution in the HVR were not consistent with the random accumulation of mutations and imply that amino acid replacement in the HVR was strongly constrained. Another variable region of E2 centered on codon 60 shows similar constraints, while HVR2 was relatively unconstrained. Several of these features are difficult to explain if a neutralizing immune response against the HVR is the only selective force operating on E2. The impact of PCR artifacts such as nucleotide misincorporation and the shuffling of dissimilar templates is discussed.

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Year:  1998        PMID: 9573256      PMCID: PMC110045          DOI: 10.1128/JVI.72.6.4893-4905.1998

Source DB:  PubMed          Journal:  J Virol        ISSN: 0022-538X            Impact factor:   5.103


  52 in total

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4.  Dynamic analysis of heterogeneous hepatitis C virus populations by direct solid-phase sequencing.

Authors:  J Odeberg; Z Yun; A Sönnerborg; M Uhlén; J Lundeberg
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5.  Molecular epidemiology of an outbreak of infection with hepatitis C virus in recipients of anti-D immunoglobulin.

Authors:  J P Power; E Lawlor; F Davidson; E C Holmes; P L Yap; P Simmonds
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6.  Occurrence of antibodies reactive with more than one variant of the putative envelope glycoprotein (gp70) hypervariable region 1 in viremic hepatitis C virus-infected patients.

Authors:  E Scarselli; A Cerino; G Esposito; E Silini; M U Mondelli; C Traboni
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Authors:  A Zibert; E Schreier; M Roggendorf
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8.  Quasispecies of hepatitis C virus and genetic drift of the hypervariable region in chronic type C hepatitis.

Authors:  J H Kao; P J Chen; M Y Lai; T H Wang; D S Chen
Journal:  J Infect Dis       Date:  1995-07       Impact factor: 5.226

9.  Comparison of full-length sequences of interferon-sensitive and resistant hepatitis C virus 1b. Sensitivity to interferon is conferred by amino acid substitutions in the NS5A region.

Authors:  N Enomoto; I Sakuma; Y Asahina; M Kurosaki; T Murakami; C Yamamoto; N Izumi; F Marumo; C Sato
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Review 10.  Variability of hepatitis C virus.

Authors:  P Simmonds
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2.  Conservation of the conformation and positive charges of hepatitis C virus E2 envelope glycoprotein hypervariable region 1 points to a role in cell attachment.

Authors:  F Penin; C Combet; G Germanidis; P O Frainais; G Deléage; J M Pawlotsky
Journal:  J Virol       Date:  2001-06       Impact factor: 5.103

Review 3.  Viral quasispecies evolution.

Authors:  Esteban Domingo; Julie Sheldon; Celia Perales
Journal:  Microbiol Mol Biol Rev       Date:  2012-06       Impact factor: 11.056

4.  Hypervariable region 1 sequence stability during hepatitis C virus replication in chimpanzees.

Authors:  S C Ray; Q Mao; R E Lanford; S Bassett; O Laeyendecker; Y M Wang; D L Thomas
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5.  Hepatitis C hypervariable region 1: association of reduced selection pressure in african americans with treatment failure.

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7.  Evolutionary rate and genetic drift of hepatitis C virus are not correlated with the host immune response: studies of infected donor-recipient clusters.

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Review 10.  Managing occupational risks for hepatitis C transmission in the health care setting.

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