Cutaneous Immunization Rapidly Activates Liver Invariant Vα14 NKT Cells Stimulating B-1 B Cells to Initiate T Cell Recruitment for Elicitation of Contact Sensitivity

T cell recruitment to elicit contact sensitivity (CS) requires a CS-initiating process mediated by B-1 cells that produce IgM, which activates complement to promote T cell passage into the tissues. We now show that Vα14i NKT cells induce B-1 cell activation likely by releasing IL-4 early postimmuniz...

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Autores principales: Campos, Regis A., Szczepanik, Marian, Itakura, Atsuko, Akahira-Azuma, Moe, Sidobre, Stephane, Kronenberg, Mitchell, Askenase, Philip W.
Formato: Texto
Lenguaje:English
Publicado: The Rockefeller University Press 2003
Materias:
Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2194147/
https://www.ncbi.nlm.nih.gov/pubmed/14676294
http://dx.doi.org/10.1084/jem.20021562
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author Campos, Regis A.
Szczepanik, Marian
Itakura, Atsuko
Akahira-Azuma, Moe
Sidobre, Stephane
Kronenberg, Mitchell
Askenase, Philip W.
author_facet Campos, Regis A.
Szczepanik, Marian
Itakura, Atsuko
Akahira-Azuma, Moe
Sidobre, Stephane
Kronenberg, Mitchell
Askenase, Philip W.
author_sort Campos, Regis A.
collection PubMed
description T cell recruitment to elicit contact sensitivity (CS) requires a CS-initiating process mediated by B-1 cells that produce IgM, which activates complement to promote T cell passage into the tissues. We now show that Vα14i NKT cells induce B-1 cell activation likely by releasing IL-4 early postimmunization. The CS initiation process is absent in Jα18(−/−) and CD1d(−/−) NKT cell–deficient mice and is reconstituted by populations enriched for Vα14i NKT cells. Transfers are not effective if cells are derived from IL-4(−/−) mice. Staining with specific tetramers directly showed that hepatic Vα14i NKT cells increase by 30 min and nearly double by 2 h postimmunization. Transfer of immune B-1 cells also reconstitutes CS responses in NKT cell–deficient mice. The B-1 cells act downstream of the Vα14i NKT cells to restore CS initiation. In addition, IL-4 given systemically to Jα18(−/−) or CD1d(−/−) NKT cell–deficient mice reconstitutes elicitation of CS. Further, splenocytes from immune Jα18(−/−) mice produce less antigen (Ag)-specific IgM antibodies compared with sensitized WT mice. Together these findings indicate that very early after skin immunization Vα14i NKT cells are stimulated to produce IL-4, which activates B-1 cells to produce Ag-specific IgM, subsequently needed to recruit effector T cells for elicitation of CS responses.
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spelling pubmed-21941472008-04-11 Cutaneous Immunization Rapidly Activates Liver Invariant Vα14 NKT Cells Stimulating B-1 B Cells to Initiate T Cell Recruitment for Elicitation of Contact Sensitivity Campos, Regis A. Szczepanik, Marian Itakura, Atsuko Akahira-Azuma, Moe Sidobre, Stephane Kronenberg, Mitchell Askenase, Philip W. J Exp Med Article T cell recruitment to elicit contact sensitivity (CS) requires a CS-initiating process mediated by B-1 cells that produce IgM, which activates complement to promote T cell passage into the tissues. We now show that Vα14i NKT cells induce B-1 cell activation likely by releasing IL-4 early postimmunization. The CS initiation process is absent in Jα18(−/−) and CD1d(−/−) NKT cell–deficient mice and is reconstituted by populations enriched for Vα14i NKT cells. Transfers are not effective if cells are derived from IL-4(−/−) mice. Staining with specific tetramers directly showed that hepatic Vα14i NKT cells increase by 30 min and nearly double by 2 h postimmunization. Transfer of immune B-1 cells also reconstitutes CS responses in NKT cell–deficient mice. The B-1 cells act downstream of the Vα14i NKT cells to restore CS initiation. In addition, IL-4 given systemically to Jα18(−/−) or CD1d(−/−) NKT cell–deficient mice reconstitutes elicitation of CS. Further, splenocytes from immune Jα18(−/−) mice produce less antigen (Ag)-specific IgM antibodies compared with sensitized WT mice. Together these findings indicate that very early after skin immunization Vα14i NKT cells are stimulated to produce IL-4, which activates B-1 cells to produce Ag-specific IgM, subsequently needed to recruit effector T cells for elicitation of CS responses. The Rockefeller University Press 2003-12-15 /pmc/articles/PMC2194147/ /pubmed/14676294 http://dx.doi.org/10.1084/jem.20021562 Text en Copyright © 2003, 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
Campos, Regis A.
Szczepanik, Marian
Itakura, Atsuko
Akahira-Azuma, Moe
Sidobre, Stephane
Kronenberg, Mitchell
Askenase, Philip W.
Cutaneous Immunization Rapidly Activates Liver Invariant Vα14 NKT Cells Stimulating B-1 B Cells to Initiate T Cell Recruitment for Elicitation of Contact Sensitivity
title Cutaneous Immunization Rapidly Activates Liver Invariant Vα14 NKT Cells Stimulating B-1 B Cells to Initiate T Cell Recruitment for Elicitation of Contact Sensitivity
title_full Cutaneous Immunization Rapidly Activates Liver Invariant Vα14 NKT Cells Stimulating B-1 B Cells to Initiate T Cell Recruitment for Elicitation of Contact Sensitivity
title_fullStr Cutaneous Immunization Rapidly Activates Liver Invariant Vα14 NKT Cells Stimulating B-1 B Cells to Initiate T Cell Recruitment for Elicitation of Contact Sensitivity
title_full_unstemmed Cutaneous Immunization Rapidly Activates Liver Invariant Vα14 NKT Cells Stimulating B-1 B Cells to Initiate T Cell Recruitment for Elicitation of Contact Sensitivity
title_short Cutaneous Immunization Rapidly Activates Liver Invariant Vα14 NKT Cells Stimulating B-1 B Cells to Initiate T Cell Recruitment for Elicitation of Contact Sensitivity
title_sort cutaneous immunization rapidly activates liver invariant vα14 nkt cells stimulating b-1 b cells to initiate t cell recruitment for elicitation of contact sensitivity
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2194147/
https://www.ncbi.nlm.nih.gov/pubmed/14676294
http://dx.doi.org/10.1084/jem.20021562
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