The immune response of BALB/c mice to influenza hemagglutinin: commonality of the B cell and T cell repertoires and their relevance to antigenic drift

BC Barnett, CM Graham, DS Burt… - European journal of …, 1989 - Wiley Online Library
BC Barnett, CM Graham, DS Burt, JJ Skehel, D Brian Thomas
European journal of immunology, 1989Wiley Online Library
An extensive analysis of the class II (I‐Ad)‐restricted T cell repertoire for influenza
hemagglutinin (HA) of the H3 subtype, elicited by natural infection, has shown that a majority
of CD4 memory T cell clones focus on antibody‐binding regions of HA, sites B and E, and
are sensitive to the residue substitutions that have occurred in these regions during
antigenic drift. The proliferative responses of CD4 clones to synthetic peptides have
identified T cell epitopes within site B, HA1 177–199 and HA1 182–199, and site E, HA1 56 …
Abstract
An extensive analysis of the class II (I‐Ad)‐restricted T cell repertoire for influenza hemagglutinin (HA) of the H3 subtype, elicited by natural infection, has shown that a majority of CD4 memory T cell clones focus on antibody‐binding regions of HA, sites B and E, and are sensitive to the residue substitutions that have occurred in these regions during antigenic drift. The proliferative responses of CD4 clones to synthetic peptides have identified T cell epitopes within site B, HA1 177–199 and HA1 182–199, and site E, HA1 56–76. The recognition specificity of T cell clones for antibody‐selected mutant viruses, with single amino acid substitutions within these recognition sites identified residues 63, 189, 193 and 198 as being important for T cell recognition and thus established that BALB/c, CD4 T cell clones were sensitive to the same substitutions known to abrogate BALB/c antibody recognition of the native HA. Our findings indicate extensive commonality of the B cell and T cell repertoires for HA, which may be relevant to an understanding of the immune pressures for antigenic drift, and, moreover, suggest that the antigen‐specific B memory cell may be instrumental in selection of the peripheral T cell repertoire.
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