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Tissue-Specific Education of Decidual NK Cells

During human pregnancy, fetal trophoblast cells invade the decidua and remodel maternal spiral arteries to establish adequate nutrition during gestation. Tissue NK cells in the decidua (dNK) express inhibitory NK receptors (iNKR) that recognize allogeneic HLA-C molecules on trophoblast. Where this r...

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Autores principales: Sharkey, Andrew M., Xiong, Shiqiu, Kennedy, Philippa R., Gardner, Lucy, Farrell, Lydia E., Chazara, Olympe, Ivarsson, Martin A., Hiby, Susan E., Colucci, Francesco, Moffett, Ashley
Formato: Online Artículo Texto
Lenguaje:English
Publicado: AAI 2015
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4574523/
https://www.ncbi.nlm.nih.gov/pubmed/26320253
http://dx.doi.org/10.4049/jimmunol.1501229
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author Sharkey, Andrew M.
Xiong, Shiqiu
Kennedy, Philippa R.
Gardner, Lucy
Farrell, Lydia E.
Chazara, Olympe
Ivarsson, Martin A.
Hiby, Susan E.
Colucci, Francesco
Moffett, Ashley
author_facet Sharkey, Andrew M.
Xiong, Shiqiu
Kennedy, Philippa R.
Gardner, Lucy
Farrell, Lydia E.
Chazara, Olympe
Ivarsson, Martin A.
Hiby, Susan E.
Colucci, Francesco
Moffett, Ashley
author_sort Sharkey, Andrew M.
collection PubMed
description During human pregnancy, fetal trophoblast cells invade the decidua and remodel maternal spiral arteries to establish adequate nutrition during gestation. Tissue NK cells in the decidua (dNK) express inhibitory NK receptors (iNKR) that recognize allogeneic HLA-C molecules on trophoblast. Where this results in excessive dNK inhibition, the risk of pre-eclampsia or growth restriction is increased. However, the role of maternal, self–HLA-C in regulating dNK responsiveness is unknown. We investigated how the expression and function of five iNKR in dNK is influenced by maternal HLA-C. In dNK isolated from women who have HLA-C alleles that carry a C2 epitope, there is decreased expression frequency of the cognate receptor, KIR2DL1. In contrast, women with HLA-C alleles bearing a C1 epitope have increased frequency of the corresponding receptor, KIR2DL3. Maternal HLA-C had no significant effect on KIR2DL1 or KIR2DL3 in peripheral blood NK cells (pbNK). This resulted in a very different KIR repertoire for dNK capable of binding C1 or C2 epitopes compared with pbNK. We also show that, although maternal KIR2DL1 binding to C2 epitope educates dNK cells to acquire functional competence, the effects of other iNKR on dNK responsiveness are quite different from those in pbNK. This provides a basis for understanding how dNK responses to allogeneic trophoblast affect the outcome of pregnancy. Our findings suggest that the mechanisms that determine the repertoire of iNKR and the effect of self-MHC on NK education may differ in tissue NK cells compared with pbNK.
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spelling pubmed-45745232015-09-22 Tissue-Specific Education of Decidual NK Cells Sharkey, Andrew M. Xiong, Shiqiu Kennedy, Philippa R. Gardner, Lucy Farrell, Lydia E. Chazara, Olympe Ivarsson, Martin A. Hiby, Susan E. Colucci, Francesco Moffett, Ashley J Immunol Clinical and Human Immunology During human pregnancy, fetal trophoblast cells invade the decidua and remodel maternal spiral arteries to establish adequate nutrition during gestation. Tissue NK cells in the decidua (dNK) express inhibitory NK receptors (iNKR) that recognize allogeneic HLA-C molecules on trophoblast. Where this results in excessive dNK inhibition, the risk of pre-eclampsia or growth restriction is increased. However, the role of maternal, self–HLA-C in regulating dNK responsiveness is unknown. We investigated how the expression and function of five iNKR in dNK is influenced by maternal HLA-C. In dNK isolated from women who have HLA-C alleles that carry a C2 epitope, there is decreased expression frequency of the cognate receptor, KIR2DL1. In contrast, women with HLA-C alleles bearing a C1 epitope have increased frequency of the corresponding receptor, KIR2DL3. Maternal HLA-C had no significant effect on KIR2DL1 or KIR2DL3 in peripheral blood NK cells (pbNK). This resulted in a very different KIR repertoire for dNK capable of binding C1 or C2 epitopes compared with pbNK. We also show that, although maternal KIR2DL1 binding to C2 epitope educates dNK cells to acquire functional competence, the effects of other iNKR on dNK responsiveness are quite different from those in pbNK. This provides a basis for understanding how dNK responses to allogeneic trophoblast affect the outcome of pregnancy. Our findings suggest that the mechanisms that determine the repertoire of iNKR and the effect of self-MHC on NK education may differ in tissue NK cells compared with pbNK. AAI 2015-10-01 2015-08-28 /pmc/articles/PMC4574523/ /pubmed/26320253 http://dx.doi.org/10.4049/jimmunol.1501229 Text en Copyright © 2015 The Authors This is an open-access article distributed under the terms of the CC-BY 3.0 Unported license.
spellingShingle Clinical and Human Immunology
Sharkey, Andrew M.
Xiong, Shiqiu
Kennedy, Philippa R.
Gardner, Lucy
Farrell, Lydia E.
Chazara, Olympe
Ivarsson, Martin A.
Hiby, Susan E.
Colucci, Francesco
Moffett, Ashley
Tissue-Specific Education of Decidual NK Cells
title Tissue-Specific Education of Decidual NK Cells
title_full Tissue-Specific Education of Decidual NK Cells
title_fullStr Tissue-Specific Education of Decidual NK Cells
title_full_unstemmed Tissue-Specific Education of Decidual NK Cells
title_short Tissue-Specific Education of Decidual NK Cells
title_sort tissue-specific education of decidual nk cells
topic Clinical and Human Immunology
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC4574523/
https://www.ncbi.nlm.nih.gov/pubmed/26320253
http://dx.doi.org/10.4049/jimmunol.1501229
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