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Antigenic relevance of F protein in chronic hepatitis C virus infection
Author(s) -
KomurianPradel Florence,
Rajoharison Alain,
Berland JeanLuc,
Khouri Valérie,
Perret Magali,
Van Roosmalen Mark,
Pol Stanislas,
Negro Francesco,
ParanhosBaccalà Glaucia
Publication year - 2004
Publication title -
hepatology
Language(s) - English
Resource type - Journals
SCImago Journal Rank - 5.488
H-Index - 361
eISSN - 1527-3350
pISSN - 0270-9139
DOI - 10.1002/hep.1840400420
Subject(s) - virology , antigen , hepatitis a virus , hepatitis b antigens , virus , medicine , biology , immunology , hepatitis b virus
The hepatitis C virus (HCV) F protein is a recently described, frameshift product of HCV core encoding sequence of genotype 1a. Its function and antigenic properties are unknown. Using enzyme‐linked immunosorbent assay, we assessed the prevalence of anti‐F antibodies in 154 patients chronically infected with HCV, 65 patients with other liver diseases, and 121 healthy controls. For this purpose, we expressed a highly purified HCV F recombinant protein from HCV genotype 1a in Escherichia coli. Because the F protein shares the 10 first amino acids with the core protein, the anti‐HCV F response was also assessed by a F recombinant protein deleted of its 10 first amino acids [Δ(1‐10)‐F]. Ninety‐six (62%) of the 154 HCV serum samples reacted with the complete F recombinant protein, whereas 39 (25%) showed a weaker anti‐Δ(1‐10)F reactivity and 150 (97%) had anti‐core antibodies. No reactivity against F, Δ(1‐10)F, or core was detected in any of the controls. To exclude a potential cross‐reaction of anti‐F antibodies with anti‐core antibodies, a specific enzyme‐linked immunosorbent assay was performed for anti‐core antibodies. The specificity of anti‐F antibodies was confirmed using an F synthetic peptide. The prevalence of anti‐F antibodies did not correlate with HCV RNA serum level, genotype, or stage of liver disease. Sequence analysis from 8 anti‐F–‐positive and 5 anti‐F–‐negative serum samples did not reveal any particular difference potentially accounting for their respective anti‐F responses. In conclusion, the F protein elicits specific antibodies in 62% of individuals chronically infected with HCV; such anti‐F response does not seem to be affected by the F sequence heterogeneity. (Hepatology 2004;40:900‐909).