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Three Distinct Subsets of Thymic Epithelial Cells in Rats and Mice Defined by Novel Antibodies

AIM: Thymic epithelial cells (TECs) are thought to play an essential role in T cell development and have been detected mainly in mice using lectin binding and antibodies to keratins. Our aim in the present study was to create a precise map of rat TECs using antibodies to putative markers and novel m...

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Autores principales: Sawanobori, Yasushi, Ueta, Hiashi, Dijkstra, Christine D., Park, Chae Gyu, Satou, Motoyasu, Kitazawa, Yusuke, Matsuno, Kenjiro
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2014
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4204869/
https://www.ncbi.nlm.nih.gov/pubmed/25334032
http://dx.doi.org/10.1371/journal.pone.0109995
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author Sawanobori, Yasushi
Ueta, Hiashi
Dijkstra, Christine D.
Park, Chae Gyu
Satou, Motoyasu
Kitazawa, Yusuke
Matsuno, Kenjiro
author_facet Sawanobori, Yasushi
Ueta, Hiashi
Dijkstra, Christine D.
Park, Chae Gyu
Satou, Motoyasu
Kitazawa, Yusuke
Matsuno, Kenjiro
author_sort Sawanobori, Yasushi
collection PubMed
description AIM: Thymic epithelial cells (TECs) are thought to play an essential role in T cell development and have been detected mainly in mice using lectin binding and antibodies to keratins. Our aim in the present study was to create a precise map of rat TECs using antibodies to putative markers and novel monoclonal antibodies (i.e., ED 18/19/21 and anti-CD205 antibodies) and compare it with a map from mouse counterparts and that of rat thymic dendritic cells. RESULTS: Rat TECs were subdivided on the basis of phenotype into three subsets; ED18(+)ED19(+/−)keratin 5 (K5)(+)K8(+)CD205(+) class II MHC (MHCII)(+) cortical TECs (cTECs), ED18(+)ED21(−)K5(−)K8(+) Ulex europaeus lectin 1 (UEA-1)(+)CD205(−) medullary TECs (mTEC1s), and ED18(+)ED21(+)K5(+)K8(dull)UEA-1(−)CD205(−) medullary TECs (mTEC2s). Thymic nurse cells were defined in cytosmears as an ED18(+)ED19(+/−)K5(+)K8(+) subset of cTECs. mTEC1s preferentially expressed MHCII, claudin-3, claudin-4, and autoimmune regulator (AIRE). Use of ED18 and ED21 antibodies revealed three subsets of TECs in mice as well. We also detected two distinct TEC-free areas in the subcapsular cortex and in the medulla. Rat dendritic cells in the cortex were MHCII(+)CD103(+) but negative for TEC markers, including CD205. Those in the medulla were MHCII(+)CD103(+) and CD205(+) cells were found only in the TEC-free area. CONCLUSION: Both rats and mice have three TEC subsets with similar phenotypes that can be identified using known markers and new monoclonal antibodies. These findings will facilitate further analysis of TEC subsets and DCs and help to define their roles in thymic selection and in pathological states such as autoimmune disorders.
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spelling pubmed-42048692014-10-27 Three Distinct Subsets of Thymic Epithelial Cells in Rats and Mice Defined by Novel Antibodies Sawanobori, Yasushi Ueta, Hiashi Dijkstra, Christine D. Park, Chae Gyu Satou, Motoyasu Kitazawa, Yusuke Matsuno, Kenjiro PLoS One Research Article AIM: Thymic epithelial cells (TECs) are thought to play an essential role in T cell development and have been detected mainly in mice using lectin binding and antibodies to keratins. Our aim in the present study was to create a precise map of rat TECs using antibodies to putative markers and novel monoclonal antibodies (i.e., ED 18/19/21 and anti-CD205 antibodies) and compare it with a map from mouse counterparts and that of rat thymic dendritic cells. RESULTS: Rat TECs were subdivided on the basis of phenotype into three subsets; ED18(+)ED19(+/−)keratin 5 (K5)(+)K8(+)CD205(+) class II MHC (MHCII)(+) cortical TECs (cTECs), ED18(+)ED21(−)K5(−)K8(+) Ulex europaeus lectin 1 (UEA-1)(+)CD205(−) medullary TECs (mTEC1s), and ED18(+)ED21(+)K5(+)K8(dull)UEA-1(−)CD205(−) medullary TECs (mTEC2s). Thymic nurse cells were defined in cytosmears as an ED18(+)ED19(+/−)K5(+)K8(+) subset of cTECs. mTEC1s preferentially expressed MHCII, claudin-3, claudin-4, and autoimmune regulator (AIRE). Use of ED18 and ED21 antibodies revealed three subsets of TECs in mice as well. We also detected two distinct TEC-free areas in the subcapsular cortex and in the medulla. Rat dendritic cells in the cortex were MHCII(+)CD103(+) but negative for TEC markers, including CD205. Those in the medulla were MHCII(+)CD103(+) and CD205(+) cells were found only in the TEC-free area. CONCLUSION: Both rats and mice have three TEC subsets with similar phenotypes that can be identified using known markers and new monoclonal antibodies. These findings will facilitate further analysis of TEC subsets and DCs and help to define their roles in thymic selection and in pathological states such as autoimmune disorders. Public Library of Science 2014-10-21 /pmc/articles/PMC4204869/ /pubmed/25334032 http://dx.doi.org/10.1371/journal.pone.0109995 Text en © 2014 Sawanobori 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
Sawanobori, Yasushi
Ueta, Hiashi
Dijkstra, Christine D.
Park, Chae Gyu
Satou, Motoyasu
Kitazawa, Yusuke
Matsuno, Kenjiro
Three Distinct Subsets of Thymic Epithelial Cells in Rats and Mice Defined by Novel Antibodies
title Three Distinct Subsets of Thymic Epithelial Cells in Rats and Mice Defined by Novel Antibodies
title_full Three Distinct Subsets of Thymic Epithelial Cells in Rats and Mice Defined by Novel Antibodies
title_fullStr Three Distinct Subsets of Thymic Epithelial Cells in Rats and Mice Defined by Novel Antibodies
title_full_unstemmed Three Distinct Subsets of Thymic Epithelial Cells in Rats and Mice Defined by Novel Antibodies
title_short Three Distinct Subsets of Thymic Epithelial Cells in Rats and Mice Defined by Novel Antibodies
title_sort three distinct subsets of thymic epithelial cells in rats and mice defined by novel antibodies
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4204869/
https://www.ncbi.nlm.nih.gov/pubmed/25334032
http://dx.doi.org/10.1371/journal.pone.0109995
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