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Natural Killer Cell Signal Integration Balances Synapse Symmetry and Migration

Natural killer (NK) cells discern the health of other cells by recognising the balance of activating and inhibitory ligands expressed by each target cell. However, how the integration of activating and inhibitory signals relates to formation of the NK cell immune synapse remains a central question i...

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Autores principales: Culley, Fiona J., Johnson, Matthew, Evans, J. Henry, Kumar, Sunil, Crilly, Rupert, Casasbuenas, Juan, Schnyder, Tim, Mehrabi, Maryam, Deonarain, Mahendra P., Ushakov, Dmitry S., Braud, Veronique, Roth, Günter, Brock, Roland, Köhler, Karsten, Davis, Daniel M.
Formato: Texto
Lenguaje:English
Publicado: Public Library of Science 2009
Materias:
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2707003/
https://www.ncbi.nlm.nih.gov/pubmed/19636352
http://dx.doi.org/10.1371/journal.pbio.1000159
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author Culley, Fiona J.
Johnson, Matthew
Evans, J. Henry
Kumar, Sunil
Crilly, Rupert
Casasbuenas, Juan
Schnyder, Tim
Mehrabi, Maryam
Deonarain, Mahendra P.
Ushakov, Dmitry S.
Braud, Veronique
Roth, Günter
Brock, Roland
Köhler, Karsten
Davis, Daniel M.
author_facet Culley, Fiona J.
Johnson, Matthew
Evans, J. Henry
Kumar, Sunil
Crilly, Rupert
Casasbuenas, Juan
Schnyder, Tim
Mehrabi, Maryam
Deonarain, Mahendra P.
Ushakov, Dmitry S.
Braud, Veronique
Roth, Günter
Brock, Roland
Köhler, Karsten
Davis, Daniel M.
author_sort Culley, Fiona J.
collection PubMed
description Natural killer (NK) cells discern the health of other cells by recognising the balance of activating and inhibitory ligands expressed by each target cell. However, how the integration of activating and inhibitory signals relates to formation of the NK cell immune synapse remains a central question in our understanding of NK cell recognition. Here we report that ligation of LFA-1 on NK cells induced asymmetrical cell spreading and migration. In contrast, ligation of the activating receptor NKG2D induced symmetrical spreading of ruffled lamellipodia encompassing a dynamic ring of f-actin, concurrent with polarization towards a target cell and a “stop” signal. Ligation of both LFA-1 and NKG2D together resulted in symmetrical spreading but co-ligation of inhibitory receptors reverted NK cells to an asymmetrical migratory configuration leading to inhibitory synapses being smaller and more rapidly disassembled. Using micropatterned activating and inhibitory ligands, signals were found to be continuously and locally integrated during spreading. Together, these data demonstrate that NK cells spread to form large, stable, symmetrical synapses if activating signals dominate, whereas asymmetrical migratory “kinapses” are favoured if inhibitory signals dominate. This clarifies how the integration of activating and inhibitory receptor signals is translated to an appropriate NK cell response.
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spelling pubmed-27070032009-07-28 Natural Killer Cell Signal Integration Balances Synapse Symmetry and Migration Culley, Fiona J. Johnson, Matthew Evans, J. Henry Kumar, Sunil Crilly, Rupert Casasbuenas, Juan Schnyder, Tim Mehrabi, Maryam Deonarain, Mahendra P. Ushakov, Dmitry S. Braud, Veronique Roth, Günter Brock, Roland Köhler, Karsten Davis, Daniel M. PLoS Biol Research Article Natural killer (NK) cells discern the health of other cells by recognising the balance of activating and inhibitory ligands expressed by each target cell. However, how the integration of activating and inhibitory signals relates to formation of the NK cell immune synapse remains a central question in our understanding of NK cell recognition. Here we report that ligation of LFA-1 on NK cells induced asymmetrical cell spreading and migration. In contrast, ligation of the activating receptor NKG2D induced symmetrical spreading of ruffled lamellipodia encompassing a dynamic ring of f-actin, concurrent with polarization towards a target cell and a “stop” signal. Ligation of both LFA-1 and NKG2D together resulted in symmetrical spreading but co-ligation of inhibitory receptors reverted NK cells to an asymmetrical migratory configuration leading to inhibitory synapses being smaller and more rapidly disassembled. Using micropatterned activating and inhibitory ligands, signals were found to be continuously and locally integrated during spreading. Together, these data demonstrate that NK cells spread to form large, stable, symmetrical synapses if activating signals dominate, whereas asymmetrical migratory “kinapses” are favoured if inhibitory signals dominate. This clarifies how the integration of activating and inhibitory receptor signals is translated to an appropriate NK cell response. Public Library of Science 2009-07-28 /pmc/articles/PMC2707003/ /pubmed/19636352 http://dx.doi.org/10.1371/journal.pbio.1000159 Text en Culley 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
Culley, Fiona J.
Johnson, Matthew
Evans, J. Henry
Kumar, Sunil
Crilly, Rupert
Casasbuenas, Juan
Schnyder, Tim
Mehrabi, Maryam
Deonarain, Mahendra P.
Ushakov, Dmitry S.
Braud, Veronique
Roth, Günter
Brock, Roland
Köhler, Karsten
Davis, Daniel M.
Natural Killer Cell Signal Integration Balances Synapse Symmetry and Migration
title Natural Killer Cell Signal Integration Balances Synapse Symmetry and Migration
title_full Natural Killer Cell Signal Integration Balances Synapse Symmetry and Migration
title_fullStr Natural Killer Cell Signal Integration Balances Synapse Symmetry and Migration
title_full_unstemmed Natural Killer Cell Signal Integration Balances Synapse Symmetry and Migration
title_short Natural Killer Cell Signal Integration Balances Synapse Symmetry and Migration
title_sort natural killer cell signal integration balances synapse symmetry and migration
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC2707003/
https://www.ncbi.nlm.nih.gov/pubmed/19636352
http://dx.doi.org/10.1371/journal.pbio.1000159
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