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Functional Differences between Human NKp44(−) and NKp44(+) RORC(+) Innate Lymphoid Cells

Human RORC(+) lymphoid tissue inducer cells are part of a rapidly expanding family of innate lymphoid cells (ILC) that participate in innate and adaptive immune responses as well as in lymphoid tissue (re) modeling. The assessment of a potential role for innate lymphocyte-derived cytokines in human...

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Autores principales: Hoorweg, Kerim, Peters, Charlotte P., Cornelissen, Ferry, Aparicio-Domingo, Patricia, Papazian, Natalie, Kazemier, Geert, Mjösberg, Jenny M., Spits, Hergen, Cupedo, Tom
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Frontiers Research Foundation 2012
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3342004/
https://www.ncbi.nlm.nih.gov/pubmed/22566953
http://dx.doi.org/10.3389/fimmu.2012.00072
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author Hoorweg, Kerim
Peters, Charlotte P.
Cornelissen, Ferry
Aparicio-Domingo, Patricia
Papazian, Natalie
Kazemier, Geert
Mjösberg, Jenny M.
Spits, Hergen
Cupedo, Tom
author_facet Hoorweg, Kerim
Peters, Charlotte P.
Cornelissen, Ferry
Aparicio-Domingo, Patricia
Papazian, Natalie
Kazemier, Geert
Mjösberg, Jenny M.
Spits, Hergen
Cupedo, Tom
author_sort Hoorweg, Kerim
collection PubMed
description Human RORC(+) lymphoid tissue inducer cells are part of a rapidly expanding family of innate lymphoid cells (ILC) that participate in innate and adaptive immune responses as well as in lymphoid tissue (re) modeling. The assessment of a potential role for innate lymphocyte-derived cytokines in human homeostasis and disease is hampered by a poor characterization of RORC(+) innate cell subsets and a lack of knowledge on the distribution of these cells in adults. Here we show that functionally distinct subsets of human RORC(+) innate lymphoid cells are enriched for secretion of IL-17a or IL-22. Both subsets have an activated phenotype and can be distinguished based on the presence or absence of the natural cytotoxicity receptor NKp44. NKp44(+) IL-22 producing cells are present in tonsils while NKp44(−) IL-17a producing cells are present in fetal developing lymph nodes. Development of human intestinal NKp44(+) ILC is a programmed event that is independent of bacterial colonization and these cells colonize the fetal intestine during the first trimester. In the adult intestine, NKp44(+) ILC are the main ILC subset producing IL-22. NKp44(−) ILC remain present throughout adulthood in peripheral non-inflamed lymph nodes as resting, non-cytokine producing cells. However, upon stimulation lymph node ILC can swiftly initiate cytokine transcription suggesting that secondary human lymphoid organs may function as a reservoir for innate lymphoid cells capable of participating in inflammatory responses.
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spelling pubmed-33420042012-05-07 Functional Differences between Human NKp44(−) and NKp44(+) RORC(+) Innate Lymphoid Cells Hoorweg, Kerim Peters, Charlotte P. Cornelissen, Ferry Aparicio-Domingo, Patricia Papazian, Natalie Kazemier, Geert Mjösberg, Jenny M. Spits, Hergen Cupedo, Tom Front Immunol Immunology Human RORC(+) lymphoid tissue inducer cells are part of a rapidly expanding family of innate lymphoid cells (ILC) that participate in innate and adaptive immune responses as well as in lymphoid tissue (re) modeling. The assessment of a potential role for innate lymphocyte-derived cytokines in human homeostasis and disease is hampered by a poor characterization of RORC(+) innate cell subsets and a lack of knowledge on the distribution of these cells in adults. Here we show that functionally distinct subsets of human RORC(+) innate lymphoid cells are enriched for secretion of IL-17a or IL-22. Both subsets have an activated phenotype and can be distinguished based on the presence or absence of the natural cytotoxicity receptor NKp44. NKp44(+) IL-22 producing cells are present in tonsils while NKp44(−) IL-17a producing cells are present in fetal developing lymph nodes. Development of human intestinal NKp44(+) ILC is a programmed event that is independent of bacterial colonization and these cells colonize the fetal intestine during the first trimester. In the adult intestine, NKp44(+) ILC are the main ILC subset producing IL-22. NKp44(−) ILC remain present throughout adulthood in peripheral non-inflamed lymph nodes as resting, non-cytokine producing cells. However, upon stimulation lymph node ILC can swiftly initiate cytokine transcription suggesting that secondary human lymphoid organs may function as a reservoir for innate lymphoid cells capable of participating in inflammatory responses. Frontiers Research Foundation 2012-04-09 /pmc/articles/PMC3342004/ /pubmed/22566953 http://dx.doi.org/10.3389/fimmu.2012.00072 Text en Copyright © 2012 Hoorweg, Peters, Cornelissen, Aparicio-Domingo, Papazian, Kazemier, Mjösberg, Spits and Cupedo. http://www.frontiersin.org/licenseagreement This is an open-access article distributed under the terms of the Creative Commons Attribution Non Commercial License, which permits non-commercial use, distribution, and reproduction in other forums, provided the original authors and source are credited.
spellingShingle Immunology
Hoorweg, Kerim
Peters, Charlotte P.
Cornelissen, Ferry
Aparicio-Domingo, Patricia
Papazian, Natalie
Kazemier, Geert
Mjösberg, Jenny M.
Spits, Hergen
Cupedo, Tom
Functional Differences between Human NKp44(−) and NKp44(+) RORC(+) Innate Lymphoid Cells
title Functional Differences between Human NKp44(−) and NKp44(+) RORC(+) Innate Lymphoid Cells
title_full Functional Differences between Human NKp44(−) and NKp44(+) RORC(+) Innate Lymphoid Cells
title_fullStr Functional Differences between Human NKp44(−) and NKp44(+) RORC(+) Innate Lymphoid Cells
title_full_unstemmed Functional Differences between Human NKp44(−) and NKp44(+) RORC(+) Innate Lymphoid Cells
title_short Functional Differences between Human NKp44(−) and NKp44(+) RORC(+) Innate Lymphoid Cells
title_sort functional differences between human nkp44(−) and nkp44(+) rorc(+) innate lymphoid cells
topic Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC3342004/
https://www.ncbi.nlm.nih.gov/pubmed/22566953
http://dx.doi.org/10.3389/fimmu.2012.00072
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