Immunoresponses to Neisseria Meningitidis Epitopes: Immunomodulation by Meningococcus B Acts on More Than One Meningococcal Surface Epitope

Overview

Journal Med Microbiol Immunol

Specialty Allergy & Immunology

Date 1987 Jan 1

PMID 2439885

Citations 1

Authors

J Faro

R Seoane

I Lareo

A Eiras

J Couceiro

B J Regueiro

Affiliations

Soon will be listed here.

Abstract

Neisseria meningitidis group B strain M986 (serotypes 2a, 7) (NMB) elicits a specific primary antiphosphorylcholine immune response in mice but not a secondary response. The ability of other serotype and serogroup meningococci to induce similar primary responses in mice was studied, as was the immunogenicity of trinitrophenyl coupled NMB (TNP-NMB) in primary and secondary antitrinitrophenyl responses. Except for NMB, all other strains tested (three serogroup B and one serogroup A meningococcal strains) were found to be very poor phosphorylcholine immunogens. TNP-NMB, however, though proving to be a very good TNP antigen, was only a weak phosphorylcholine antigen. Priming NBF1 female mice with TNP-NMB one month or more before challenging them with the same antigen induced a strong depression of anti-TNP response in the subsequent challenge. However, this effect was not observed with Xid NBF1 male mice. Furthermore, priming mice with NMB weakly affected the anti-TNP response, but greatly depressed the antiphosphorylcholine response, after TNP-NMB challenge. In addition, whereas apparently only one TNP-specific B cell subpopulation was responding in unprimed mice challenged simultaneously with TNP-NMB and TNP-Ficoll (non-additive response), priming mice with NMB appeared to facilitate the independent activation of two different TNP-specific B cell subpopulations (additive response).

Citing Articles

Immunoresponses to Neisseria meningitidis epitopes: in vivo analysis of immunocompetent cells involved in suppression of secondary response to phosphorylcholine.

Faro J, Seoane R, Lareo I, Eiras A, Schiller M, Regueiro B Med Microbiol Immunol. 1987; 176(6):289-303.

PMID: 2448596 DOI: 10.1007/BF00194889.

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