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Journal of Clinical Microbiology, 12 1997, 3062-3070, Vol 35, No. 12
JA Neville, LE Prescott, V Bhattacherjee, N Adams, I Pike, B Rodgers, A El- Zayadi, S Hamid, GM Dusheiko, AA Saeed, GH Haydon and P Simmonds
Assays that detect antibody to hepatitis C virus (HCV) are used to screen
blood donors and patients with hepatitis. Current enzyme-linked
immunosorbent assay (ELISA)-based methods are invariably based upon
antigens from expressed recombinant proteins or oligopeptides from HCV type
1. Some HCV antigens used in screening assays are coded by regions of the
HCV genome that show extensive variability; therefore, HCV type 1-based
assays may be less effective for the detection of antibody elicited by
infection with other genotypes. In this study, we have measured antibody
reactivity of sera from 110 hepatitis C patients infected with type 1b, 3a,
or 4a to genotype-specific and cross- reactive epitopes present in
recombinant proteins from HCV genotypes 1b (core, NS3, and NS5), 3a (NS3,
NS5), and 4a (core, NS3), corresponding to those used in current
third-generation screening ELISAs. By comparing the serological
reactivities of sera to type-homologous and type-heterologous antigens, we
detected a significant type-specific component to the reactivity to NS3 (61
to 77% of the total reactivity) and NS5 (60% of the total reactivity).
Furthermore, despite the similarities in the amino acid sequences of the
core antigens of type 1b and type 4a, we also found significantly greater
reactivity to type- homologous antigens, with approximately 25% of
reactivity being type specific. These findings are consistent with previous
findings of fivefold weaker reactivity of sera from HCV type 2- and HCV
type 3- infected blood donors in the currently used third-generation ELISAs
and suggest that these assays are suboptimal for screening populations in
which the predominant genotype is not type 1.
Copyright © 1997 by the American Society for Microbiology. All rights reserved.
Antigenic variation of core, NS3, and NS5 proteins among genotypes of hepatitis C virus [In Process Citation]
Department of Medical Microbiology, University of Edinburgh, United Kingdom.
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