Sero-reactivity to three distinct regions within the hepatitis C virus alternative reading frame protein (ARFP/core+1) in patients with chronic HCV genotype-3 infection

Elsheikh, Mosaab E. A.; Patrick McClure, C.; Tarr, Alexander W.; Irving, William L.

doi:10.1099/jgv.0.001727

Sero-reactivity to three distinct regions within the hepatitis C virus alternative reading frame protein (ARFP/core+1) in patients with chronic HCV genotype-3 infection

Elsheikh, Mosaab E. A.; Patrick McClure, C.; Tarr, Alexander W.; Irving, William L.

Authors

Mosaab E. A. Elsheikh

PATRICK MCCLURE PATRICK.MCCLURE@NOTTINGHAM.AC.UK
Assistant Professor

ALEXANDER TARR alex.tarr@nottingham.ac.uk
Associate Professor

WILLIAM IRVING mrzwi@nottingham.ac.uk
Professor of Virology

Abstract

Hepatitis C virus (HCV) infection affects more than 71 million people worldwide. The disease slowly progresses to chronic, long-term liver injury which leads to hepatocellular carcinoma (HCC) in 5 % of infections. The alternative reading frame protein (ARFP/core+1) is encoded by a sequence overlapping the HCV core gene in the +1 reading frame. Its role in hepatitis C pathogenesis and the viral life cycle is unclear, although some observers have related its production to disease progression and the development of HCC. The aim of this study was to determine whether ARFP is immunogenic in patients with chronic HCV genotype 3 infection and to assess whether sero-reactivity is associated with disease progression, particularly to HCC. Immunogenic epitopes within the protein were predicted by a bioinformatics tool, and three -20 aa length-peptides (ARFP-P1, ARFP-P2 and ARFP-P3) were synthesized and used in an avidin-biotin ARFP/core+1 peptide ELISA. Serum samples from 50 patients with chronic HCV genotype 3 infection, 50 genotype-1 patients, 50 HBV patients and 110 healthy controls were tested. Sero-reactivity to the ARFP peptides was also tested and compared in 114 chronic HCV genotype-3 patients subdivided on the basis of disease severity into non-cirrhotic, cirrhotic and HCC groups. Chronic HCV genotype-3 patients showed noticeable rates of reactivity to ARFP and core peptides. Seropositivity rates were 58% for ARFP-P1, 47 % for ARFP-P2, 5.9 % for ARFP-P3 and 100 % for C22 peptides. There was no significant difference between these seroreactivities between HCV genotype-3 patients with HCC, and HCV genotype-3 patients with and without liver cirrhosis. Patients with chronic HCV genotype-3 infection frequently produce antibodies against ARFP/core+1 protein. ARFP peptide reactivity was not associated with disease severity in patients with HCV genotype-3. These results support the conclusion that ARFP/core+1 is produced during HCV infection, but they do not confirm that antibodies to ARFP can indicate HCV disease progression.

Citation

Elsheikh, M. E. A., Patrick McClure, C., Tarr, A. W., & Irving, W. L. (2022). Sero-reactivity to three distinct regions within the hepatitis C virus alternative reading frame protein (ARFP/core+1) in patients with chronic HCV genotype-3 infection. Journal of General Virology, 103(3), Article 001727. https://doi.org/10.1099/jgv.0.001727

Journal Article Type	Article
Acceptance Date	Dec 9, 2021
Online Publication Date	Mar 1, 2022
Publication Date	Mar 1, 2022
Deposit Date	Dec 10, 2021
Publicly Available Date	Mar 1, 2022
Journal	Journal of General Virology
Print ISSN	0022-1317
Electronic ISSN	1465-2099
Publisher	Microbiology Society
Peer Reviewed	Peer Reviewed
Volume	103
Issue	3
Article Number	001727
DOI	https://doi.org/10.1099/jgv.0.001727
Keywords	Virology
Public URL	https://nottingham-repository.worktribe.com/output/6916644
Publisher URL	https://www.microbiologyresearch.org/content/journal/jgv/10.1099/jgv.0.001727

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Sero-reactivity to three distinct regions within the hepatitis C virus alternative reading frame protein (ARFP/core+1) in patients with chronic HCV genotype-3 infection (1.4 Mb)
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