## Abstract Hepatitis B virus (HBV) e antigen (HBeAg) seroconversion during chronic HBV infection is known to play an important role in disease progression and patient response to antiviral agents. The aim of the present study was to analyze gender disparity in distribution of major hydrophilic reg
Characterization of minor and major antigenic regions within the hepatitis B virus nucleocapsid
✍ Scribed by Marc Tordjeman; Gilles Fontan; Véronique Rabillon; Jacques Martin; Christian Trepo; Agnés Hoffenbach; Kamel Mabrouk; Jean Marc Sabatier; Jurphaas van Rietschoten; Gérard Somme
- Publisher
- John Wiley and Sons
- Year
- 1993
- Tongue
- English
- Weight
- 902 KB
- Volume
- 41
- Category
- Article
- ISSN
- 0146-6615
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✦ Synopsis
Abstract
Hepatitis B core antibodies (anti‐HBc) appear very early during the course of the hepatitis B virus infection and often persist years after viral clearance. In order to characterize the immunodominant domain of the HBcAg, the human immune response against the HBV nucleocapsid (HBcAg) was analyzed by using 14 synthetic peptides. Anti‐HBc antibodies were detected by an indirect enzyme‐linked immunosorbent assay (ELISA) with HBc peptides. Results suggest that the anti‐HBc response is heterogeneous and directed against the whole primary structure of the HBc protein. Results also indicate that the epitopes recognized by anti‐HBc antibodies can vary with the stages of the disease. In most sera from patients with serological evidence of acute HBV infection, anti‐HBc antibodies recognized all the HBc peptides; conversely, after the acute phase, anti‐HBc antibodies recognized predominantly epitopes located within the central region of the HBc protein from residue 74 to 123. Our results suggest that the HBV core protein is made up of two antigenic regions: a major one expressing a family of immunodominant epitopes from residue 74 to 123, whereas the minor encompasses the rest of the protein. The concept of the conformational nature of the unique HBcAg determinant is discussed, suggesting numerous families of linear epitopes.
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