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Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model

The kinetics of antigen-presenting cells (APCs) vary depending on their resident tissues and the manner of immunization. We investigated the long-term changes in mature APC and T-cell subsets over 4 weeks in the ocular surface in murine models of corneal quiescent or potent sterile inflammation, and...

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Autores principales: Kim, Kyoung-Woo, Lee, Hyun-Ju, Kim, Hyeon-Ji, Kim, Mee-Kum
Formato: Online Artículo Texto
Lenguaje:English
Publicado: MDPI 2021
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8467177/
https://www.ncbi.nlm.nih.gov/pubmed/34571859
http://dx.doi.org/10.3390/cells10092210
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author Kim, Kyoung-Woo
Lee, Hyun-Ju
Kim, Hyeon-Ji
Kim, Mee-Kum
author_facet Kim, Kyoung-Woo
Lee, Hyun-Ju
Kim, Hyeon-Ji
Kim, Mee-Kum
author_sort Kim, Kyoung-Woo
collection PubMed
description The kinetics of antigen-presenting cells (APCs) vary depending on their resident tissues and the manner of immunization. We investigated the long-term changes in mature APC and T-cell subsets over 4 weeks in the ocular surface in murine models of corneal quiescent or potent sterile inflammation, and allosensitization using partial (PT), syngeneic (Syn), and allogeneic (Allo) corneal transplantation. In PT, CD11b(int)CD11c(hi)MHCII(hi)CD86(hi) cells increased until 4 weeks with an increase in IFNγ(hi) T cells. In Syn, both CD11b(int)CD11c(hi)MHCII(hi)CD86(hi) and CD11b(hi)CD11c(hi)MHCII(hi)CD86(hi) APC subsets increased until 4 weeks with a brief increase in CD69(hi) T cells at 2 weeks. In Allo, CD11b(int)CD11c(hi)MHCII(hi)CD86(hi) and CD11b(hi)CD11c(hi)MHCII(hi)CD86(hi) APC subsets increased until 4 weeks, and an early increase in CD69(hi) T cells was observed at 2 weeks followed by a late increase in IFNγ(hi) T cells at 4 weeks. The frequency of the IFNγ(hi) T cell subset was positively correlated with the frequency of the CD11b(int)CD11c(hi)MHCII(hi)CD86(hi) subset, indicating the existence of APC–T cell interaction in the ocular surface. Together, the results indicate that allosensitization in mature APCs leads to T-cell activation in the ocular surface, whereas sterile inflammation merely induces a brief and non-specific T-cell activation in the ocular surface.
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spelling pubmed-84671772021-09-27 Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model Kim, Kyoung-Woo Lee, Hyun-Ju Kim, Hyeon-Ji Kim, Mee-Kum Cells Article The kinetics of antigen-presenting cells (APCs) vary depending on their resident tissues and the manner of immunization. We investigated the long-term changes in mature APC and T-cell subsets over 4 weeks in the ocular surface in murine models of corneal quiescent or potent sterile inflammation, and allosensitization using partial (PT), syngeneic (Syn), and allogeneic (Allo) corneal transplantation. In PT, CD11b(int)CD11c(hi)MHCII(hi)CD86(hi) cells increased until 4 weeks with an increase in IFNγ(hi) T cells. In Syn, both CD11b(int)CD11c(hi)MHCII(hi)CD86(hi) and CD11b(hi)CD11c(hi)MHCII(hi)CD86(hi) APC subsets increased until 4 weeks with a brief increase in CD69(hi) T cells at 2 weeks. In Allo, CD11b(int)CD11c(hi)MHCII(hi)CD86(hi) and CD11b(hi)CD11c(hi)MHCII(hi)CD86(hi) APC subsets increased until 4 weeks, and an early increase in CD69(hi) T cells was observed at 2 weeks followed by a late increase in IFNγ(hi) T cells at 4 weeks. The frequency of the IFNγ(hi) T cell subset was positively correlated with the frequency of the CD11b(int)CD11c(hi)MHCII(hi)CD86(hi) subset, indicating the existence of APC–T cell interaction in the ocular surface. Together, the results indicate that allosensitization in mature APCs leads to T-cell activation in the ocular surface, whereas sterile inflammation merely induces a brief and non-specific T-cell activation in the ocular surface. MDPI 2021-08-26 /pmc/articles/PMC8467177/ /pubmed/34571859 http://dx.doi.org/10.3390/cells10092210 Text en © 2021 by the authors. https://creativecommons.org/licenses/by/4.0/Licensee MDPI, Basel, Switzerland. This article is an open access article distributed under the terms and conditions of the Creative Commons Attribution (CC BY) license (https://creativecommons.org/licenses/by/4.0/).
spellingShingle Article
Kim, Kyoung-Woo
Lee, Hyun-Ju
Kim, Hyeon-Ji
Kim, Mee-Kum
Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model
title Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model
title_full Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model
title_fullStr Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model
title_full_unstemmed Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model
title_short Time-Dependent Serial Changes of Antigen-Presenting Cell Subsets in the Ocular Surface Are Distinct between Corneal Sterile Inflammation and Allosensitization in a Murine Model
title_sort time-dependent serial changes of antigen-presenting cell subsets in the ocular surface are distinct between corneal sterile inflammation and allosensitization in a murine model
topic Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC8467177/
https://www.ncbi.nlm.nih.gov/pubmed/34571859
http://dx.doi.org/10.3390/cells10092210
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