A TRANSMISSIBLE GASTROENTERITIS CORONAVIRUS NUCLEOPROTEIN EPITOPE ELICITS T-HELPER CELLS THAT COLLABORATE IN THE IN-VITRO ANTIBODY-SYNTHESIS TO THE 3 MAJOR STRUCTURAL VIRAL-PROTEINS
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作者:
ANTON, IM
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机构:CENT VET INST, 8200 AB LELYSTAD, NETHERLANDS
ANTON, IM
SUNE, C
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机构:CENT VET INST, 8200 AB LELYSTAD, NETHERLANDS
SUNE, C
MELOEN, RH
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机构:CENT VET INST, 8200 AB LELYSTAD, NETHERLANDS
MELOEN, RH
BORRASCUESTA, F
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机构:CENT VET INST, 8200 AB LELYSTAD, NETHERLANDS
BORRASCUESTA, F
ENJUANES, L
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机构:CENT VET INST, 8200 AB LELYSTAD, NETHERLANDS
ENJUANES, L
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[1] CENT VET INST, 8200 AB LELYSTAD, NETHERLANDS
[2] UNIV NAVARRA, DEPT MED INTERNA, E-31080 PAMPLONA, SPAIN
Four strong T cell epitopes have been identified studying the blastogenic response of lymphocytes from haplotype-defined transmissible gastroenteritis virus (TGEV) immune miniswine to sixty-one 15-mer synthetic peptides. Three of these epitopes are located on the nucleoprotein (N-46, amino acids 46 to 60; N-272, amino acids 272 to 286; and N-321, amino acids 321 to 335), and one on the membrane protein (M(196), amino acids 196 to 210). N-321, peptide induced the highest T cell response and was recognized by immune miniswine lymphocytes with haplotypes dd, aa, and cc, T lymphocytes from peptide N321(-) immune miniswine reconstituted the in vitro synthesis of TGEV-specific antibodies by complementing CD4(-) TGEV-immune cells. This response was directed at least against the three major structural proteins. The synthesized antibodies specific for S protein preferentially recognized discontinous epitopes and neutralized TGEV infectivity. These results show that peptide N-321 defines a functional T helper epitope eliciting T cells capable of collaborating with B cells specific for different proteins of TGEV. (C) 1995 Academic Press, Inc.