Apoptosis in mesenchymal stromal cells induces in vivo recipient-mediated immunomodulation
Apoptosis in mesenchymal stromal cells induces in vivo recipient-mediated immunomodulation
The immunosuppressive activity of mesenchymal stromal cells (MSCs) is well documented. However, the therapeutic benefit is completely unpredictable, thus raising concerns about MSC efficacy. One of the affecting factors is the unresolved conundrum that, despite being immunosuppressive, MSCs are undetectable after administration. Therefore, understanding the fate of infused MSCs could help predict clinical responses. Using a murine model of graft-versus-host disease (GvHD), we demonstrate that MSCs are actively induced to undergo perforin-dependent apoptosis by recipient cytotoxic cells and that this process is essential to initiate MSC-induced immunosuppression. When examining patients with GvHD who received MSCs, we found a striking parallel, whereby only those with high cytotoxic activity against MSCs responded to MSC infusion, whereas those with low activity did not. The need for recipient cytotoxic cell activity could be replaced by the infusion of apoptotic MSCs generated ex vivo. After infusion, recipient phagocytes engulf apoptotic MSCs and produce indoleamine 2,3-dioxygenase, which is ultimately necessary for effecting immunosuppression. Therefore, we propose the innovative concept that patients should be stratified for MSC treatment according to their ability to kill MSCs or that all patients could be treated with ex vivo apoptotic MSCs.
Journal Article
Galleu, Antonio
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Riffo-Vasquez, Yanira
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Trento, Cristina
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Lomas, Cara
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Dolcetti, Luigi
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Cheung, Tik Shing
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von Bonin, Malte
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Barbieri, Laura
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Halai, Krishma
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Ward, Sophie
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Weng, Ling
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Chakraverty, Ronjon
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Lombardi, Giovanna
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Watt, Fiona M.
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Orchard, Kim
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Marks, David I
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Apperley, Jane
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Bornhauser, Martin
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Walczak, Henning
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Bennett, Clare
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Dazzi, Francesco
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15 November 2017
Galleu, Antonio
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Riffo-Vasquez, Yanira
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Trento, Cristina
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Lomas, Cara
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Dolcetti, Luigi
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Cheung, Tik Shing
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von Bonin, Malte
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Barbieri, Laura
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Halai, Krishma
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Ward, Sophie
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Weng, Ling
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Chakraverty, Ronjon
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Lombardi, Giovanna
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Watt, Fiona M.
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Orchard, Kim
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Marks, David I
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Apperley, Jane
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Bornhauser, Martin
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Walczak, Henning
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Bennett, Clare
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Dazzi, Francesco
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Galleu, Antonio, Riffo-Vasquez, Yanira, Trento, Cristina, Lomas, Cara, Dolcetti, Luigi, Cheung, Tik Shing, von Bonin, Malte, Barbieri, Laura, Halai, Krishma, Ward, Sophie, Weng, Ling, Chakraverty, Ronjon, Lombardi, Giovanna, Watt, Fiona M., Orchard, Kim, Marks, David I, Apperley, Jane, Bornhauser, Martin, Walczak, Henning, Bennett, Clare and Dazzi, Francesco
(2017)
Apoptosis in mesenchymal stromal cells induces in vivo recipient-mediated immunomodulation.
Science Translational Medicine, 9 (416), [eaam7828].
(doi:10.1126/scitranslmed.aam7828).
Abstract
The immunosuppressive activity of mesenchymal stromal cells (MSCs) is well documented. However, the therapeutic benefit is completely unpredictable, thus raising concerns about MSC efficacy. One of the affecting factors is the unresolved conundrum that, despite being immunosuppressive, MSCs are undetectable after administration. Therefore, understanding the fate of infused MSCs could help predict clinical responses. Using a murine model of graft-versus-host disease (GvHD), we demonstrate that MSCs are actively induced to undergo perforin-dependent apoptosis by recipient cytotoxic cells and that this process is essential to initiate MSC-induced immunosuppression. When examining patients with GvHD who received MSCs, we found a striking parallel, whereby only those with high cytotoxic activity against MSCs responded to MSC infusion, whereas those with low activity did not. The need for recipient cytotoxic cell activity could be replaced by the infusion of apoptotic MSCs generated ex vivo. After infusion, recipient phagocytes engulf apoptotic MSCs and produce indoleamine 2,3-dioxygenase, which is ultimately necessary for effecting immunosuppression. Therefore, we propose the innovative concept that patients should be stratified for MSC treatment according to their ability to kill MSCs or that all patients could be treated with ex vivo apoptotic MSCs.
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Accepted/In Press date: 16 August 2017
e-pub ahead of print date: 15 November 2017
Published date: 15 November 2017
Keywords:
Journal Article
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Local EPrints ID: 416432
URI: http://eprints.soton.ac.uk/id/eprint/416432
ISSN: 1946-6234
PURE UUID: c8f56caf-0c97-4d3b-85af-1e1a837a8615
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Date deposited: 15 Dec 2017 17:31
Last modified: 16 Mar 2024 03:26
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Contributors
Author:
Antonio Galleu
Author:
Yanira Riffo-Vasquez
Author:
Cristina Trento
Author:
Cara Lomas
Author:
Luigi Dolcetti
Author:
Tik Shing Cheung
Author:
Malte von Bonin
Author:
Laura Barbieri
Author:
Krishma Halai
Author:
Sophie Ward
Author:
Ling Weng
Author:
Ronjon Chakraverty
Author:
Giovanna Lombardi
Author:
Fiona M. Watt
Author:
Kim Orchard
Author:
David I Marks
Author:
Jane Apperley
Author:
Martin Bornhauser
Author:
Henning Walczak
Author:
Clare Bennett
Author:
Francesco Dazzi
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