M tuberculosis in the Adjuvant Modulates Time of Appearance of CNS-Specific Effector T Cells in the Spleen through a Polymorphic Site of TLR2

DC deliver information regulating trafficking of effector T cells along T-cell priming. However, the role of pathogen-derived motives in the regulation of movement of T cells has not been studied. We hereinafter report that amount of M tuberculosis in the adjuvant modulates relocation of PLP139-151...

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Autores principales: Nicolò, Chiara, Di Sante, Gabriele, Procoli, Annabella, Migliara, Giuseppe, Piermattei, Alessia, Valentini, Mariagrazia, Delogu, Giovanni, Cittadini, Achille, Constantin, Gabriela, Ria, Francesco
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2013
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3569447/
https://www.ncbi.nlm.nih.gov/pubmed/23409051
http://dx.doi.org/10.1371/journal.pone.0055819
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author Nicolò, Chiara
Di Sante, Gabriele
Procoli, Annabella
Migliara, Giuseppe
Piermattei, Alessia
Valentini, Mariagrazia
Delogu, Giovanni
Cittadini, Achille
Constantin, Gabriela
Ria, Francesco
author_facet Nicolò, Chiara
Di Sante, Gabriele
Procoli, Annabella
Migliara, Giuseppe
Piermattei, Alessia
Valentini, Mariagrazia
Delogu, Giovanni
Cittadini, Achille
Constantin, Gabriela
Ria, Francesco
author_sort Nicolò, Chiara
collection PubMed
description DC deliver information regulating trafficking of effector T cells along T-cell priming. However, the role of pathogen-derived motives in the regulation of movement of T cells has not been studied. We hereinafter report that amount of M tuberculosis in the adjuvant modulates relocation of PLP139-151 specific T cells. In the presence of a low dose of M tuberculosis in the adjuvant, T cells (detected by CDR3 BV-BJ spectratyping, the so-called “immunoscope”) mostly reach the spleen by day 28 after immunization (“late relocation”) in the SJL strain, whereas T cells reach the spleen by d 14 with a high dose of M tuberculosis (“early relocation”). The C57Bl/6 background confers a dominant “early relocation” phenotype to F1 (SJL×C57Bl/6) mice, allowing early relocation of T cells in the presence of low dose M tuberculosis. A single non-synonymous polymorphism of TLR2 is responsible for “early/late” relocation phenotype. Egress of T lymphocytes is regulated by TLR2 expressed on T cells. Thus, pathogens engaging TLR2 on T cells regulate directly T-cell trafficking, and polymorphisms of TLR2 condition T-cell trafficking upon a limiting concentration of ligand.
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spelling pubmed-35694472013-02-13 M tuberculosis in the Adjuvant Modulates Time of Appearance of CNS-Specific Effector T Cells in the Spleen through a Polymorphic Site of TLR2 Nicolò, Chiara Di Sante, Gabriele Procoli, Annabella Migliara, Giuseppe Piermattei, Alessia Valentini, Mariagrazia Delogu, Giovanni Cittadini, Achille Constantin, Gabriela Ria, Francesco PLoS One Research Article DC deliver information regulating trafficking of effector T cells along T-cell priming. However, the role of pathogen-derived motives in the regulation of movement of T cells has not been studied. We hereinafter report that amount of M tuberculosis in the adjuvant modulates relocation of PLP139-151 specific T cells. In the presence of a low dose of M tuberculosis in the adjuvant, T cells (detected by CDR3 BV-BJ spectratyping, the so-called “immunoscope”) mostly reach the spleen by day 28 after immunization (“late relocation”) in the SJL strain, whereas T cells reach the spleen by d 14 with a high dose of M tuberculosis (“early relocation”). The C57Bl/6 background confers a dominant “early relocation” phenotype to F1 (SJL×C57Bl/6) mice, allowing early relocation of T cells in the presence of low dose M tuberculosis. A single non-synonymous polymorphism of TLR2 is responsible for “early/late” relocation phenotype. Egress of T lymphocytes is regulated by TLR2 expressed on T cells. Thus, pathogens engaging TLR2 on T cells regulate directly T-cell trafficking, and polymorphisms of TLR2 condition T-cell trafficking upon a limiting concentration of ligand. Public Library of Science 2013-02-11 /pmc/articles/PMC3569447/ /pubmed/23409051 http://dx.doi.org/10.1371/journal.pone.0055819 Text en © 2013 Nicolò et al http://creativecommons.org/licenses/by/4.0/ This is an open-access article distributed under the terms of the Creative Commons Attribution License, which permits unrestricted use, distribution, and reproduction in any medium, provided the original author and source are properly credited.
spellingShingle Research Article
Nicolò, Chiara
Di Sante, Gabriele
Procoli, Annabella
Migliara, Giuseppe
Piermattei, Alessia
Valentini, Mariagrazia
Delogu, Giovanni
Cittadini, Achille
Constantin, Gabriela
Ria, Francesco
M tuberculosis in the Adjuvant Modulates Time of Appearance of CNS-Specific Effector T Cells in the Spleen through a Polymorphic Site of TLR2
title M tuberculosis in the Adjuvant Modulates Time of Appearance of CNS-Specific Effector T Cells in the Spleen through a Polymorphic Site of TLR2
title_full M tuberculosis in the Adjuvant Modulates Time of Appearance of CNS-Specific Effector T Cells in the Spleen through a Polymorphic Site of TLR2
title_fullStr M tuberculosis in the Adjuvant Modulates Time of Appearance of CNS-Specific Effector T Cells in the Spleen through a Polymorphic Site of TLR2
title_full_unstemmed M tuberculosis in the Adjuvant Modulates Time of Appearance of CNS-Specific Effector T Cells in the Spleen through a Polymorphic Site of TLR2
title_short M tuberculosis in the Adjuvant Modulates Time of Appearance of CNS-Specific Effector T Cells in the Spleen through a Polymorphic Site of TLR2
title_sort m tuberculosis in the adjuvant modulates time of appearance of cns-specific effector t cells in the spleen through a polymorphic site of tlr2
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3569447/
https://www.ncbi.nlm.nih.gov/pubmed/23409051
http://dx.doi.org/10.1371/journal.pone.0055819
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