Short-term IL-15 priming leaves a long-lasting signalling imprint in mouse NK cells independently of a metabolic switch

IL-15 priming of NK cells is a broadly accepted concept, but the dynamics and underlying molecular mechanisms remain poorly understood. We show that as little as 5 min of IL-15 treatment in vitro, followed by removal of excess cytokines, results in a long-lasting, but reversible, augmentation of NK...

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Autores principales: Luu, Thuy T, Schmied, Laurent, Nguyen, Ngoc-Anh, Wiel, Clotilde, Meinke, Stephan, Mohammad, Dara K, Bergö, Martin, Alici, Evren, Kadri, Nadir, Ganesan, Sridharan, Höglund, Petter
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Life Science Alliance LLC 2021
Materias:
Research Articles
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7918643/
https://www.ncbi.nlm.nih.gov/pubmed/33593878
http://dx.doi.org/10.26508/lsa.202000723
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author Luu, Thuy T
Schmied, Laurent
Nguyen, Ngoc-Anh
Wiel, Clotilde
Meinke, Stephan
Mohammad, Dara K
Bergö, Martin
Alici, Evren
Kadri, Nadir
Ganesan, Sridharan
Höglund, Petter
author_facet Luu, Thuy T
Schmied, Laurent
Nguyen, Ngoc-Anh
Wiel, Clotilde
Meinke, Stephan
Mohammad, Dara K
Bergö, Martin
Alici, Evren
Kadri, Nadir
Ganesan, Sridharan
Höglund, Petter
author_sort Luu, Thuy T
collection PubMed
description IL-15 priming of NK cells is a broadly accepted concept, but the dynamics and underlying molecular mechanisms remain poorly understood. We show that as little as 5 min of IL-15 treatment in vitro, followed by removal of excess cytokines, results in a long-lasting, but reversible, augmentation of NK cell responsiveness upon activating receptor cross-linking. In contrast to long-term stimulation, improved NK cell function after short-term IL-15 priming was not associated with enhanced metabolism but was based on the increased steady-state phosphorylation level of signalling molecules downstream of activating receptors. Inhibition of JAK3 eliminated this priming effect, suggesting a cross talk between the IL-15 receptor and ITAM-dependent activating receptors. Increased signalling molecule phosphorylation levels, calcium flux, and IFN-γ secretion lasted for up to 3 h after IL-15 stimulation before returning to baseline. We conclude that IL-15 rapidly and reversibly primes NK cell function by modulating activating receptor signalling. Our findings suggest a mechanism by which NK cell reactivity can potentially be maintained in vivo based on only brief encounters with IL-15 trans-presenting cells.
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spelling pubmed-79186432021-03-04 Short-term IL-15 priming leaves a long-lasting signalling imprint in mouse NK cells independently of a metabolic switch Luu, Thuy T Schmied, Laurent Nguyen, Ngoc-Anh Wiel, Clotilde Meinke, Stephan Mohammad, Dara K Bergö, Martin Alici, Evren Kadri, Nadir Ganesan, Sridharan Höglund, Petter Life Sci Alliance Research Articles IL-15 priming of NK cells is a broadly accepted concept, but the dynamics and underlying molecular mechanisms remain poorly understood. We show that as little as 5 min of IL-15 treatment in vitro, followed by removal of excess cytokines, results in a long-lasting, but reversible, augmentation of NK cell responsiveness upon activating receptor cross-linking. In contrast to long-term stimulation, improved NK cell function after short-term IL-15 priming was not associated with enhanced metabolism but was based on the increased steady-state phosphorylation level of signalling molecules downstream of activating receptors. Inhibition of JAK3 eliminated this priming effect, suggesting a cross talk between the IL-15 receptor and ITAM-dependent activating receptors. Increased signalling molecule phosphorylation levels, calcium flux, and IFN-γ secretion lasted for up to 3 h after IL-15 stimulation before returning to baseline. We conclude that IL-15 rapidly and reversibly primes NK cell function by modulating activating receptor signalling. Our findings suggest a mechanism by which NK cell reactivity can potentially be maintained in vivo based on only brief encounters with IL-15 trans-presenting cells. Life Science Alliance LLC 2021-02-16 /pmc/articles/PMC7918643/ /pubmed/33593878 http://dx.doi.org/10.26508/lsa.202000723 Text en © 2021 Luu et al. https://creativecommons.org/licenses/by/4.0/This article is available under a Creative Commons License (Attribution 4.0 International, as described at https://creativecommons.org/licenses/by/4.0/).
spellingShingle Research Articles
Luu, Thuy T
Schmied, Laurent
Nguyen, Ngoc-Anh
Wiel, Clotilde
Meinke, Stephan
Mohammad, Dara K
Bergö, Martin
Alici, Evren
Kadri, Nadir
Ganesan, Sridharan
Höglund, Petter
Short-term IL-15 priming leaves a long-lasting signalling imprint in mouse NK cells independently of a metabolic switch
title Short-term IL-15 priming leaves a long-lasting signalling imprint in mouse NK cells independently of a metabolic switch
title_full Short-term IL-15 priming leaves a long-lasting signalling imprint in mouse NK cells independently of a metabolic switch
title_fullStr Short-term IL-15 priming leaves a long-lasting signalling imprint in mouse NK cells independently of a metabolic switch
title_full_unstemmed Short-term IL-15 priming leaves a long-lasting signalling imprint in mouse NK cells independently of a metabolic switch
title_short Short-term IL-15 priming leaves a long-lasting signalling imprint in mouse NK cells independently of a metabolic switch
title_sort short-term il-15 priming leaves a long-lasting signalling imprint in mouse nk cells independently of a metabolic switch
topic Research Articles
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC7918643/
https://www.ncbi.nlm.nih.gov/pubmed/33593878
http://dx.doi.org/10.26508/lsa.202000723
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