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ANTIGEN RECOGNITION AND THE IMMUNE RESPONSE : "SELF-HELP" WITH SYMMETRICAL BIFUNCTIONAL ANTIGEN MOLECULES

L-Tyrosine-p-azobenzenearsonate (RAT) induces cellular immunity without humoral antibody in guinea pigs. Asymmetric bifunctional antigens composed of one RAT moiety and one dinitrophenyl (DNP) group separated by flexible spacers induce anti-RAT cellular immunity and an anti-DNP humoral response. Sym...

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Detalles Bibliográficos
Autores principales: Bush, Maurice E., Alkan, Sefik S., Nitecki, Danute E., Goodman, Joel W.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 1972
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2139336/
https://www.ncbi.nlm.nih.gov/pubmed/4118413
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author Bush, Maurice E.
Alkan, Sefik S.
Nitecki, Danute E.
Goodman, Joel W.
author_facet Bush, Maurice E.
Alkan, Sefik S.
Nitecki, Danute E.
Goodman, Joel W.
author_sort Bush, Maurice E.
collection PubMed
description L-Tyrosine-p-azobenzenearsonate (RAT) induces cellular immunity without humoral antibody in guinea pigs. Asymmetric bifunctional antigens composed of one RAT moiety and one dinitrophenyl (DNP) group separated by flexible spacers induce anti-RAT cellular immunity and an anti-DNP humoral response. Symmetrical bifunctional antigens of similar design but comprised of two RAT determinants induce cellular immunity without demonstrable anti-RAT antibody. However, when the flexible spacer is replaced by a rigid decaproline chain, humoral anti-RAT responses are provoked. Since RAT contains both electropositive (azo) and electronegative (arsonate) centers, the failure of bifunctional RAT compounds with flexible spacers to induce humoral immunity might be ascribed either to intramolecular stacking, which compromises their bifunctional character, or to interaction of both determinants with receptors on the same cell surface, which would fail to satisfy the requirement for cooperation. In order to distinguish between these alternatives, symmetrical bifunctional antigens composed of two L-tyrosine-p-azophenyltrimethylammonium (TAT) determinants separated by flexible or rigid spacers were synthesized. TAT is immunogenic and does not cross-react with RAT. Furthermore, it contains only electropositive centers and consequently bifunctional molecules do not undergo intramolecular stacking. Immunization with either flexibly or rigidly spaced bifunctional TAT antigens raised anti-TAT antibody. These results conclusively demonstrate that "self-help," cooperation between bone marrow-derived and thymus-derived lymphocytes of identical or similar specificity, can occur, provided the determinants on the antigen are prevented from associating with each other.
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spelling pubmed-21393362008-04-17 ANTIGEN RECOGNITION AND THE IMMUNE RESPONSE : "SELF-HELP" WITH SYMMETRICAL BIFUNCTIONAL ANTIGEN MOLECULES Bush, Maurice E. Alkan, Sefik S. Nitecki, Danute E. Goodman, Joel W. J Exp Med Article L-Tyrosine-p-azobenzenearsonate (RAT) induces cellular immunity without humoral antibody in guinea pigs. Asymmetric bifunctional antigens composed of one RAT moiety and one dinitrophenyl (DNP) group separated by flexible spacers induce anti-RAT cellular immunity and an anti-DNP humoral response. Symmetrical bifunctional antigens of similar design but comprised of two RAT determinants induce cellular immunity without demonstrable anti-RAT antibody. However, when the flexible spacer is replaced by a rigid decaproline chain, humoral anti-RAT responses are provoked. Since RAT contains both electropositive (azo) and electronegative (arsonate) centers, the failure of bifunctional RAT compounds with flexible spacers to induce humoral immunity might be ascribed either to intramolecular stacking, which compromises their bifunctional character, or to interaction of both determinants with receptors on the same cell surface, which would fail to satisfy the requirement for cooperation. In order to distinguish between these alternatives, symmetrical bifunctional antigens composed of two L-tyrosine-p-azophenyltrimethylammonium (TAT) determinants separated by flexible or rigid spacers were synthesized. TAT is immunogenic and does not cross-react with RAT. Furthermore, it contains only electropositive centers and consequently bifunctional molecules do not undergo intramolecular stacking. Immunization with either flexibly or rigidly spaced bifunctional TAT antigens raised anti-TAT antibody. These results conclusively demonstrate that "self-help," cooperation between bone marrow-derived and thymus-derived lymphocytes of identical or similar specificity, can occur, provided the determinants on the antigen are prevented from associating with each other. The Rockefeller University Press 1972-11-30 /pmc/articles/PMC2139336/ /pubmed/4118413 Text en Copyright © 1972 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
Bush, Maurice E.
Alkan, Sefik S.
Nitecki, Danute E.
Goodman, Joel W.
ANTIGEN RECOGNITION AND THE IMMUNE RESPONSE : "SELF-HELP" WITH SYMMETRICAL BIFUNCTIONAL ANTIGEN MOLECULES
title ANTIGEN RECOGNITION AND THE IMMUNE RESPONSE : "SELF-HELP" WITH SYMMETRICAL BIFUNCTIONAL ANTIGEN MOLECULES
title_full ANTIGEN RECOGNITION AND THE IMMUNE RESPONSE : "SELF-HELP" WITH SYMMETRICAL BIFUNCTIONAL ANTIGEN MOLECULES
title_fullStr ANTIGEN RECOGNITION AND THE IMMUNE RESPONSE : "SELF-HELP" WITH SYMMETRICAL BIFUNCTIONAL ANTIGEN MOLECULES
title_full_unstemmed ANTIGEN RECOGNITION AND THE IMMUNE RESPONSE : "SELF-HELP" WITH SYMMETRICAL BIFUNCTIONAL ANTIGEN MOLECULES
title_short ANTIGEN RECOGNITION AND THE IMMUNE RESPONSE : "SELF-HELP" WITH SYMMETRICAL BIFUNCTIONAL ANTIGEN MOLECULES
title_sort antigen recognition and the immune response : "self-help" with symmetrical bifunctional antigen molecules
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2139336/
https://www.ncbi.nlm.nih.gov/pubmed/4118413
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