Identification of immunodominant T cell epitopes of the hepatitis B virus nucleocapsid antigen. (original) (raw)
Research Article Free access | 10.1172/JCI115280
A Bertoletti, A Penna, A Cavalli, A Valli, G Missale, M Pilli, P Fowler, T Giuberti, and F V Chisari
Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Cattedra Malattie Infettive, Università di Parma, Italy.
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Published July 1, 1991 -More info
Published July 1, 1991 -Version history
Several lines of experimental evidence suggest that inclusion of core sequences in the hepatitis B vaccine may represent a feasible strategy to increase the efficacy of the vaccination. In order to identify immunodominant core epitopes, peripheral blood T cells purified from 23 patients with acute hepatitis B and different HLA haplotypes were tested with a panel of 18 short synthetic peptides (15 to 20 amino acids [AA]) covering the entire core region. All patients except one showed a strong T cell proliferative response to a single immunodominant 20 amino acid sequence located within the aminoterminal half of the core molecule. Two additional important sequences were also identified at the aminoterminal end and within the carboxyterminal half of the core molecule. These sequences were able to induce significant levels of T cell proliferation in 69 and 73% of the patients studied, respectively. T cell response to these epitopes was HLA class II restricted. The observations that (a) polyclonal T cell lines produced by PBMC stimulation with native HBcAg were specifically reactive with the relevant peptides and that (b) polyclonal T cell lines produced with synthetic peptides could be restimulated with native HBcAg, provide evidence that AA sequences contained within the synthetic peptides represent real products of the intracellular processing of the native core molecule. In conclusion, the identification of immunodominant T cell epitopes within the core molecule provides the molecular basis for the design of alternative and hopefully more immunogenic vaccines.
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