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SUPPRESSION OR AUGMENTATION OF THE ANTIHAPTEN RESPONSE IN MICE BY ANTIBODIES OF DIFFERENT SPECIFICITIES

We have measured the production by (C57 x CBA)F(1) mice of hapten-binding antibody in response to a standard dose of 50 µg of alum-precipitated NIP(12)-CG and the influence on this response of the prior administration of hyperimmune antisera raised against the homologous conjugate, the carrier globu...

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Autores principales: Haughton, G., Mäkelä, O.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1973
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2180553/
https://www.ncbi.nlm.nih.gov/pubmed/4123826
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author Haughton, G.
Mäkelä, O.
author_facet Haughton, G.
Mäkelä, O.
author_sort Haughton, G.
collection PubMed
description We have measured the production by (C57 x CBA)F(1) mice of hapten-binding antibody in response to a standard dose of 50 µg of alum-precipitated NIP(12)-CG and the influence on this response of the prior administration of hyperimmune antisera raised against the homologous conjugate, the carrier globulin alone, the hapten conjugated to a non-cross-reactive carrier (NIP(4)-OA), or a related hapten (NP) coupled to CG. The homologous antiserum was strongly immunosuppressive; a dose capable of binding about 1% of the administered hapten caused significant suppression. High doses of anticarrier serum caused significant but modest suppression (about 50%); low doses had no effect. High doses of the serum prepared against NIP(4)-OA suppressed the 19 day response by more than 97%, while 100–1,000 times lower doses caused the response to be elevated to about double the control level. The antibodies responsible for immunosuppression could be removed from this serum, as could the NIP-binding antibodies, by absorption with NIP coupled through ethylenediamine to insoluble Sepharose. The ability of this serum to augment the response was not reduced by such absorption. Augmenting antibodies could be removed by absorption with HOP-BSA-Sepharose. Thus, immunosuppression and augmentation are functions of two different populations of antibody. The former are specific hapten-binding antibodies, the latter seem to be directed against new antigenic determinants created by coupling any of the family of haptens through lysine to protein carriers. In support of this contention, it was observed that rabbit antiserum to NP-CG, after absorption with CG-Sepharose, augmented the response of mice to standard immunization with NIP(12)-CG. Female mice produced significantly more NIP-binding antibody than did males.
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spelling pubmed-21805532008-04-17 SUPPRESSION OR AUGMENTATION OF THE ANTIHAPTEN RESPONSE IN MICE BY ANTIBODIES OF DIFFERENT SPECIFICITIES Haughton, G. Mäkelä, O. J Exp Med Article We have measured the production by (C57 x CBA)F(1) mice of hapten-binding antibody in response to a standard dose of 50 µg of alum-precipitated NIP(12)-CG and the influence on this response of the prior administration of hyperimmune antisera raised against the homologous conjugate, the carrier globulin alone, the hapten conjugated to a non-cross-reactive carrier (NIP(4)-OA), or a related hapten (NP) coupled to CG. The homologous antiserum was strongly immunosuppressive; a dose capable of binding about 1% of the administered hapten caused significant suppression. High doses of anticarrier serum caused significant but modest suppression (about 50%); low doses had no effect. High doses of the serum prepared against NIP(4)-OA suppressed the 19 day response by more than 97%, while 100–1,000 times lower doses caused the response to be elevated to about double the control level. The antibodies responsible for immunosuppression could be removed from this serum, as could the NIP-binding antibodies, by absorption with NIP coupled through ethylenediamine to insoluble Sepharose. The ability of this serum to augment the response was not reduced by such absorption. Augmenting antibodies could be removed by absorption with HOP-BSA-Sepharose. Thus, immunosuppression and augmentation are functions of two different populations of antibody. The former are specific hapten-binding antibodies, the latter seem to be directed against new antigenic determinants created by coupling any of the family of haptens through lysine to protein carriers. In support of this contention, it was observed that rabbit antiserum to NP-CG, after absorption with CG-Sepharose, augmented the response of mice to standard immunization with NIP(12)-CG. Female mice produced significantly more NIP-binding antibody than did males. The Rockefeller University Press 1973-07-01 /pmc/articles/PMC2180553/ /pubmed/4123826 Text en Copyright © 1973 by The Rockefeller University Press This article is distributed under the terms of an Attribution–Noncommercial–Share Alike–No Mirror Sites license for the first six months after the publication date (see http://www.rupress.org/terms). After six months it is available under a Creative Commons License (Attribution–Noncommercial–Share Alike 4.0 Unported license, as described at http://creativecommons.org/licenses/by-nc-sa/4.0/).
spellingShingle Article
Haughton, G.
Mäkelä, O.
SUPPRESSION OR AUGMENTATION OF THE ANTIHAPTEN RESPONSE IN MICE BY ANTIBODIES OF DIFFERENT SPECIFICITIES
title SUPPRESSION OR AUGMENTATION OF THE ANTIHAPTEN RESPONSE IN MICE BY ANTIBODIES OF DIFFERENT SPECIFICITIES
title_full SUPPRESSION OR AUGMENTATION OF THE ANTIHAPTEN RESPONSE IN MICE BY ANTIBODIES OF DIFFERENT SPECIFICITIES
title_fullStr SUPPRESSION OR AUGMENTATION OF THE ANTIHAPTEN RESPONSE IN MICE BY ANTIBODIES OF DIFFERENT SPECIFICITIES
title_full_unstemmed SUPPRESSION OR AUGMENTATION OF THE ANTIHAPTEN RESPONSE IN MICE BY ANTIBODIES OF DIFFERENT SPECIFICITIES
title_short SUPPRESSION OR AUGMENTATION OF THE ANTIHAPTEN RESPONSE IN MICE BY ANTIBODIES OF DIFFERENT SPECIFICITIES
title_sort suppression or augmentation of the antihapten response in mice by antibodies of different specificities
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2180553/
https://www.ncbi.nlm.nih.gov/pubmed/4123826
work_keys_str_mv AT haughtong suppressionoraugmentationoftheantihaptenresponseinmicebyantibodiesofdifferentspecificities
AT makelao suppressionoraugmentationoftheantihaptenresponseinmicebyantibodiesofdifferentspecificities