Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a Signaling

Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a Signaling

Infection is a common and severe complication of burn injury: Sepsis accounts for 47% of postburn mortality. Burn-induced T cell suppression likely contributes to the increased infection susceptibility in burn patients. However, little is known about the kinetics of T cell dysfunction after burn and...

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Main Authors: Nadine Beckmann, Franziska Huber, Marc Hanschen, Barbara St. Pierre Schneider, Vanessa Nomellini, Charles C. Caldwell
Format: Article
Language:English
Published: Frontiers Media S.A. 2020-05-01
Series:Frontiers in Immunology
Subjects:
adaptive immunity
immunosuppression
myeloid-derived suppressor cells
immature reticulocytes
immune-checkpoint inhibitors
Online Access:https://www.frontiersin.org/article/10.3389/fimmu.2020.00876/full
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spelling doaj-19aa9d6fee704a5b9bac001411f9e91c2020-11-25T02:08:02ZengFrontiers Media S.A.Frontiers in Immunology1664-32242020-05-011110.3389/fimmu.2020.00876525219Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a SignalingNadine Beckmann0Franziska Huber1Marc Hanschen2Barbara St. Pierre Schneider3Vanessa Nomellini4Vanessa Nomellini5Charles C. Caldwell6Charles C. Caldwell7Division of Research, Department of Surgery, University of Cincinnati, Cincinnati, OH, United StatesExperimental Trauma Surgery, Klinikum Rechts der Isar, Technical University of Munich, Munich, GermanyExperimental Trauma Surgery, Klinikum Rechts der Isar, Technical University of Munich, Munich, GermanyProfessor, School of Nursing, University of Nevada, Las Vegas, NV, United StatesDivision of Research, Shriner's Hospital for Children Cincinnati, Cincinnati, OH, United StatesDivision of Trauma Critical Care and Acute Care Surgery, Department of Surgery, University of Cincinnati College of Medicine, Cincinnati, OH, United StatesDivision of Research, Department of Surgery, University of Cincinnati, Cincinnati, OH, United StatesDivision of Research, Shriner's Hospital for Children Cincinnati, Cincinnati, OH, United StatesInfection is a common and severe complication of burn injury: Sepsis accounts for 47% of postburn mortality. Burn-induced T cell suppression likely contributes to the increased infection susceptibility in burn patients. However, little is known about the kinetics of T cell dysfunction after burn and its underlying mechanisms. In this study, we show in a murine scald injury model that T cell activation of both CD4+ and CD8+ T cells as well as T cell cytokine production is suppressed acutely and persistently for at least 11 days after burn injury. Purified T cells from scald-injured mice exhibit normal T cell functions, indicating an extrinsically mediated defect. We further show that T cell dysfunction after burn appears to be cell-to-cell contact dependent and can be ameliorated by depletion of myeloid-derived suppressor cells. These cells expand after burn injury, particularly a subset expressing the checkpoint inhibitor CD172a, and infiltrate germinal centers. Expression of CD172a appears to be driven by ingestion of immature reticulocytes. Immature reticulocytes are drastically increased in the spleen of scald mice and may contribute to immunosuppression through more direct mechanisms as well. Overall, our study newly identifies two cell populations, myeloid-derived suppressor cells and immature reticulocytes, as well as the CD47/CD172a-signaling pathways as mediators of T cell suppressors after burn and thus opens up new research opportunities in the search for new therapies to combat increased infection susceptibility and the associated morbidity and mortality in burn victims.https://www.frontiersin.org/article/10.3389/fimmu.2020.00876/fulladaptive immunityimmunosuppressionmyeloid-derived suppressor cellsimmature reticulocytesimmune-checkpoint inhibitors
collection DOAJ
language English
format Article
sources DOAJ
author Nadine Beckmann
Franziska Huber
Marc Hanschen
Barbara St. Pierre Schneider
Vanessa Nomellini
Vanessa Nomellini
Charles C. Caldwell
Charles C. Caldwell
spellingShingle Nadine Beckmann
Franziska Huber
Marc Hanschen
Barbara St. Pierre Schneider
Vanessa Nomellini
Vanessa Nomellini
Charles C. Caldwell
Charles C. Caldwell
Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a Signaling
Frontiers in Immunology
adaptive immunity
immunosuppression
myeloid-derived suppressor cells
immature reticulocytes
immune-checkpoint inhibitors
author_facet Nadine Beckmann
Franziska Huber
Marc Hanschen
Barbara St. Pierre Schneider
Vanessa Nomellini
Vanessa Nomellini
Charles C. Caldwell
Charles C. Caldwell
author_sort Nadine Beckmann
title Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a Signaling
title_short Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a Signaling
title_full Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a Signaling
title_fullStr Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a Signaling
title_full_unstemmed Scald Injury-Induced T Cell Dysfunction Can Be Mitigated by Gr1+ Cell Depletion and Blockage of CD47/CD172a Signaling
title_sort scald injury-induced t cell dysfunction can be mitigated by gr1+ cell depletion and blockage of cd47/cd172a signaling
publisher Frontiers Media S.A.
series Frontiers in Immunology
issn 1664-3224
publishDate 2020-05-01
description Infection is a common and severe complication of burn injury: Sepsis accounts for 47% of postburn mortality. Burn-induced T cell suppression likely contributes to the increased infection susceptibility in burn patients. However, little is known about the kinetics of T cell dysfunction after burn and its underlying mechanisms. In this study, we show in a murine scald injury model that T cell activation of both CD4+ and CD8+ T cells as well as T cell cytokine production is suppressed acutely and persistently for at least 11 days after burn injury. Purified T cells from scald-injured mice exhibit normal T cell functions, indicating an extrinsically mediated defect. We further show that T cell dysfunction after burn appears to be cell-to-cell contact dependent and can be ameliorated by depletion of myeloid-derived suppressor cells. These cells expand after burn injury, particularly a subset expressing the checkpoint inhibitor CD172a, and infiltrate germinal centers. Expression of CD172a appears to be driven by ingestion of immature reticulocytes. Immature reticulocytes are drastically increased in the spleen of scald mice and may contribute to immunosuppression through more direct mechanisms as well. Overall, our study newly identifies two cell populations, myeloid-derived suppressor cells and immature reticulocytes, as well as the CD47/CD172a-signaling pathways as mediators of T cell suppressors after burn and thus opens up new research opportunities in the search for new therapies to combat increased infection susceptibility and the associated morbidity and mortality in burn victims.
topic adaptive immunity
immunosuppression
myeloid-derived suppressor cells
immature reticulocytes
immune-checkpoint inhibitors
url https://www.frontiersin.org/article/10.3389/fimmu.2020.00876/full
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