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Accumulation of Metal-Specific T Cells in Inflamed Skin in a Novel Murine Model of Chromium-Induced Allergic Contact Dermatitis

Chromium (Cr) causes delayed-type hypersensitivity reactions possibly mediated by accumulating T cells into allergic inflamed skin, which are called irritants or allergic contact dermatitis. However, accumulating T cells during development of metal allergy are poorly characterized because a suitable...

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Autores principales: Shigematsu, Hiroaki, Kumagai, Kenichi, Kobayashi, Hiroshi, Eguchi, Takanori, Kitaura, Kazutaka, Suzuki, Satsuki, Horikawa, Tatsuya, Matsutani, Takaji, Ogasawara, Kouetsu, Hamada, Yoshiki, Suzuki, Ryuji
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3896422/
https://www.ncbi.nlm.nih.gov/pubmed/24465826
http://dx.doi.org/10.1371/journal.pone.0085983
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author Shigematsu, Hiroaki
Kumagai, Kenichi
Kobayashi, Hiroshi
Eguchi, Takanori
Kitaura, Kazutaka
Suzuki, Satsuki
Horikawa, Tatsuya
Matsutani, Takaji
Ogasawara, Kouetsu
Hamada, Yoshiki
Suzuki, Ryuji
author_facet Shigematsu, Hiroaki
Kumagai, Kenichi
Kobayashi, Hiroshi
Eguchi, Takanori
Kitaura, Kazutaka
Suzuki, Satsuki
Horikawa, Tatsuya
Matsutani, Takaji
Ogasawara, Kouetsu
Hamada, Yoshiki
Suzuki, Ryuji
author_sort Shigematsu, Hiroaki
collection PubMed
description Chromium (Cr) causes delayed-type hypersensitivity reactions possibly mediated by accumulating T cells into allergic inflamed skin, which are called irritants or allergic contact dermatitis. However, accumulating T cells during development of metal allergy are poorly characterized because a suitable animal model is not available. This study aimed to elucidate the skewing of T-cell receptor (TCR) repertoire and cytokine profiles in accumulated T cells in inflamed skin during elucidation of Cr allergy. A novel model of Cr allergy was induced by two sensitizations of Cr plus lipopolysaccharide solution into mouse groin followed by single Cr challenge into the footpad. TCR repertoires and nucleotide sequences of complementary determining region 3 were assessed in accumulated T cells from inflamed skin. Cytokine expression profiles and T-cell phenotypes were determined by qPCR. CD3+CD4+ T cells accumulated in allergic footpads and produced increased T helper 1 (Th1) type cytokines, Fas, and Fas ligand in the footpads after challenge, suggesting CD4+ Th1 cells locally expanded in response to Cr. Accumulated T cells included natural killer (NK) T cells and Cr-specific T cells with VA11-1/VB14-1 usage, suggesting metal-specific T cells driven by invariant NKT cells might contribute to the pathogenesis of Cr allergy.
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spelling pubmed-38964222014-01-24 Accumulation of Metal-Specific T Cells in Inflamed Skin in a Novel Murine Model of Chromium-Induced Allergic Contact Dermatitis Shigematsu, Hiroaki Kumagai, Kenichi Kobayashi, Hiroshi Eguchi, Takanori Kitaura, Kazutaka Suzuki, Satsuki Horikawa, Tatsuya Matsutani, Takaji Ogasawara, Kouetsu Hamada, Yoshiki Suzuki, Ryuji PLoS One Research Article Chromium (Cr) causes delayed-type hypersensitivity reactions possibly mediated by accumulating T cells into allergic inflamed skin, which are called irritants or allergic contact dermatitis. However, accumulating T cells during development of metal allergy are poorly characterized because a suitable animal model is not available. This study aimed to elucidate the skewing of T-cell receptor (TCR) repertoire and cytokine profiles in accumulated T cells in inflamed skin during elucidation of Cr allergy. A novel model of Cr allergy was induced by two sensitizations of Cr plus lipopolysaccharide solution into mouse groin followed by single Cr challenge into the footpad. TCR repertoires and nucleotide sequences of complementary determining region 3 were assessed in accumulated T cells from inflamed skin. Cytokine expression profiles and T-cell phenotypes were determined by qPCR. CD3+CD4+ T cells accumulated in allergic footpads and produced increased T helper 1 (Th1) type cytokines, Fas, and Fas ligand in the footpads after challenge, suggesting CD4+ Th1 cells locally expanded in response to Cr. Accumulated T cells included natural killer (NK) T cells and Cr-specific T cells with VA11-1/VB14-1 usage, suggesting metal-specific T cells driven by invariant NKT cells might contribute to the pathogenesis of Cr allergy. Public Library of Science 2014-01-20 /pmc/articles/PMC3896422/ /pubmed/24465826 http://dx.doi.org/10.1371/journal.pone.0085983 Text en © 2014 Shigematsu 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
Shigematsu, Hiroaki
Kumagai, Kenichi
Kobayashi, Hiroshi
Eguchi, Takanori
Kitaura, Kazutaka
Suzuki, Satsuki
Horikawa, Tatsuya
Matsutani, Takaji
Ogasawara, Kouetsu
Hamada, Yoshiki
Suzuki, Ryuji
Accumulation of Metal-Specific T Cells in Inflamed Skin in a Novel Murine Model of Chromium-Induced Allergic Contact Dermatitis
title Accumulation of Metal-Specific T Cells in Inflamed Skin in a Novel Murine Model of Chromium-Induced Allergic Contact Dermatitis
title_full Accumulation of Metal-Specific T Cells in Inflamed Skin in a Novel Murine Model of Chromium-Induced Allergic Contact Dermatitis
title_fullStr Accumulation of Metal-Specific T Cells in Inflamed Skin in a Novel Murine Model of Chromium-Induced Allergic Contact Dermatitis
title_full_unstemmed Accumulation of Metal-Specific T Cells in Inflamed Skin in a Novel Murine Model of Chromium-Induced Allergic Contact Dermatitis
title_short Accumulation of Metal-Specific T Cells in Inflamed Skin in a Novel Murine Model of Chromium-Induced Allergic Contact Dermatitis
title_sort accumulation of metal-specific t cells in inflamed skin in a novel murine model of chromium-induced allergic contact dermatitis
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3896422/
https://www.ncbi.nlm.nih.gov/pubmed/24465826
http://dx.doi.org/10.1371/journal.pone.0085983
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