Genetic control of immune response to myoglobin. Ir gene function in genetic restriction between T and B lymphocytes.

We studied the genetic restrictions on the interaction between T cells, B cells, and antigen-presenting cells (APC) involved in the H-2-linked Ir gene control of the in vitro secondary antibody response to sperm whale myoglobin (Mb) in mice. The B cells in this study were specific for Mb itself, rat...

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Published in:Journal of Experimental Medicine
Main Authors: Kohno, Y, Berzofsky, J A
Format: Article in Journal/Newspaper
Language:English
Published: Rockefeller University Press 1982
Subjects:
Online Access:http://dx.doi.org/10.1084/jem.156.5.1486
https://rupress.org/jem/article-pdf/156/5/1486/1663228/1486.pdf
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spelling crrockefelleruni:10.1084/jem.156.5.1486 2024-06-02T08:14:54+00:00 Genetic control of immune response to myoglobin. Ir gene function in genetic restriction between T and B lymphocytes. Kohno, Y Berzofsky, J A 1982 http://dx.doi.org/10.1084/jem.156.5.1486 https://rupress.org/jem/article-pdf/156/5/1486/1663228/1486.pdf en eng Rockefeller University Press The Journal of experimental medicine volume 156, issue 5, page 1486-1501 ISSN 0022-1007 1540-9538 journal-article 1982 crrockefelleruni https://doi.org/10.1084/jem.156.5.1486 2024-05-07T14:15:40Z We studied the genetic restrictions on the interaction between T cells, B cells, and antigen-presenting cells (APC) involved in the H-2-linked Ir gene control of the in vitro secondary antibody response to sperm whale myoglobin (Mb) in mice. The B cells in this study were specific for Mb itself, rather than for a hapten unrelated to the Ir gene control, as in many previous studies. Low responder mice immunized in vivo with Mb bound to an immunogenic carrier, fowl gamma globulin (F gamma G), produced B cells competent to secrete anti-Mb antibodies in vitro if they received F gamma G-specific T cell help. However, (high-responder X low responder) F1 T cells from Mb-immune mice did not help these primed low responder (H-2k or H-2b) B cells in vitro, even in the presence of various numbers of F1 APC that were demonstrated to be component to reconstitute the response of spleen cells depleted by APC. Similar results were obtained with B6 leads to B6D2F1 radiation bone marrow chimeras. Genotypic low responder (H-2b) T cells from these mice helped Mb-primed B6D2F1B cells plus APC, but did not help syngeneic chimeric H-2b B cells, even in the presence of F1 APC. In contrast, we could not detect any Ir restriction on APC function during these in vitro secondary responses. Moreover, in the preceding paper, we found that low responder mice neonatally tolerized to higher responder H-2 had competent Mb-specific helper T cells capable of helping high responder but not low responder B cells and APC. Therefore, although function Mb-specific T cells and B cells both exist in low responder mice, the Ir gene defect is a manifestation of the failure of syngeneic collaboration between these two cell types. This genetic restriction on the interaction between T cells and B cells is consistent with the additional new finding that Lyb-5-negative B cells are a major participant in ths vitro secondary response because it is this Lyb-5-negative subpopulation of B cells that have recently been shown to require genetically restricted help. ... Article in Journal/Newspaper Sperm whale Rockefeller University Press Journal of Experimental Medicine 156 5 1486 1501
institution Open Polar
collection Rockefeller University Press
op_collection_id crrockefelleruni
language English
description We studied the genetic restrictions on the interaction between T cells, B cells, and antigen-presenting cells (APC) involved in the H-2-linked Ir gene control of the in vitro secondary antibody response to sperm whale myoglobin (Mb) in mice. The B cells in this study were specific for Mb itself, rather than for a hapten unrelated to the Ir gene control, as in many previous studies. Low responder mice immunized in vivo with Mb bound to an immunogenic carrier, fowl gamma globulin (F gamma G), produced B cells competent to secrete anti-Mb antibodies in vitro if they received F gamma G-specific T cell help. However, (high-responder X low responder) F1 T cells from Mb-immune mice did not help these primed low responder (H-2k or H-2b) B cells in vitro, even in the presence of various numbers of F1 APC that were demonstrated to be component to reconstitute the response of spleen cells depleted by APC. Similar results were obtained with B6 leads to B6D2F1 radiation bone marrow chimeras. Genotypic low responder (H-2b) T cells from these mice helped Mb-primed B6D2F1B cells plus APC, but did not help syngeneic chimeric H-2b B cells, even in the presence of F1 APC. In contrast, we could not detect any Ir restriction on APC function during these in vitro secondary responses. Moreover, in the preceding paper, we found that low responder mice neonatally tolerized to higher responder H-2 had competent Mb-specific helper T cells capable of helping high responder but not low responder B cells and APC. Therefore, although function Mb-specific T cells and B cells both exist in low responder mice, the Ir gene defect is a manifestation of the failure of syngeneic collaboration between these two cell types. This genetic restriction on the interaction between T cells and B cells is consistent with the additional new finding that Lyb-5-negative B cells are a major participant in ths vitro secondary response because it is this Lyb-5-negative subpopulation of B cells that have recently been shown to require genetically restricted help. ...
format Article in Journal/Newspaper
author Kohno, Y
Berzofsky, J A
spellingShingle Kohno, Y
Berzofsky, J A
Genetic control of immune response to myoglobin. Ir gene function in genetic restriction between T and B lymphocytes.
author_facet Kohno, Y
Berzofsky, J A
author_sort Kohno, Y
title Genetic control of immune response to myoglobin. Ir gene function in genetic restriction between T and B lymphocytes.
title_short Genetic control of immune response to myoglobin. Ir gene function in genetic restriction between T and B lymphocytes.
title_full Genetic control of immune response to myoglobin. Ir gene function in genetic restriction between T and B lymphocytes.
title_fullStr Genetic control of immune response to myoglobin. Ir gene function in genetic restriction between T and B lymphocytes.
title_full_unstemmed Genetic control of immune response to myoglobin. Ir gene function in genetic restriction between T and B lymphocytes.
title_sort genetic control of immune response to myoglobin. ir gene function in genetic restriction between t and b lymphocytes.
publisher Rockefeller University Press
publishDate 1982
url http://dx.doi.org/10.1084/jem.156.5.1486
https://rupress.org/jem/article-pdf/156/5/1486/1663228/1486.pdf
genre Sperm whale
genre_facet Sperm whale
op_source The Journal of experimental medicine
volume 156, issue 5, page 1486-1501
ISSN 0022-1007 1540-9538
op_doi https://doi.org/10.1084/jem.156.5.1486
container_title Journal of Experimental Medicine
container_volume 156
container_issue 5
container_start_page 1486
op_container_end_page 1501
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