Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells

Sepsis is a systemic infection that enhances host vulnerability to secondary infections normally controlled by T cells. Using CLP sepsis model, we observed that sepsis induces apoptosis of circulating memory CD8 T-cells (T(CIRCM)) and diminishes their effector functions, leading to impaired CD8 T-ce...

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Autores principales: Danahy, Derek B., Anthony, Scott M., Jensen, Isaac J., Hartwig, Stacey M., Shan, Qiang, Xue, Hai-Hui, Harty, John T., Griffith, Thomas S., Badovinac, Vladimir P.
Formato: Online Artículo Texto
Lenguaje:English
Publicado: Public Library of Science 2017
Materias:
Research Article
Acceso en línea:https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5599054/
https://www.ncbi.nlm.nih.gov/pubmed/28910403
http://dx.doi.org/10.1371/journal.ppat.1006569
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author Danahy, Derek B.
Anthony, Scott M.
Jensen, Isaac J.
Hartwig, Stacey M.
Shan, Qiang
Xue, Hai-Hui
Harty, John T.
Griffith, Thomas S.
Badovinac, Vladimir P.
author_facet Danahy, Derek B.
Anthony, Scott M.
Jensen, Isaac J.
Hartwig, Stacey M.
Shan, Qiang
Xue, Hai-Hui
Harty, John T.
Griffith, Thomas S.
Badovinac, Vladimir P.
author_sort Danahy, Derek B.
collection PubMed
description Sepsis is a systemic infection that enhances host vulnerability to secondary infections normally controlled by T cells. Using CLP sepsis model, we observed that sepsis induces apoptosis of circulating memory CD8 T-cells (T(CIRCM)) and diminishes their effector functions, leading to impaired CD8 T-cell mediated protection to systemic pathogen re-infection. In the context of localized re-infections, tissue resident memory CD8 T-cells (T(RM)) provide robust protection in a variety of infectious models. T(RM) rapidly ‘sense’ infection in non-lymphoid tissues and ‘alarm’ the host by enhancing immune cell recruitment to the site of the infection to accelerate pathogen clearance. Here, we show that compared to pathogen-specific T(CIRCM), sepsis does not invoke significant numerical decline of Vaccinia virus induced skin-T(RM) keeping their effector functions (e.g., Ag-dependent IFN-γ production) intact. IFN-γ-mediated recruitment of immune cells to the site of localized infection was, however, reduced in CLP hosts despite T(RM) maintaining their ‘sensing and alarming’ functions. The capacity of memory CD8 T-cells in the septic environment to respond to inflammatory cues and arrive to the site of secondary infection/antigen exposure remained normal suggesting T-cell-extrinsic factors contributed to the observed lesion. Mechanistically, we showed that IFN-γ produced rapidly during sepsis-induced cytokine storm leads to reduced IFN-γR1 expression on vascular endothelium. As a consequence, decreased expression of adhesion molecules and/or chemokines (VCAM1 and CXCL9) on skin endothelial cells in response to T(RM)-derived IFN-γ was observed, leading to sub-optimal bystander-recruitment of effector cells and increased susceptibility to pathogen re-encounter. Importantly, as visualized by intravital 2-photon microscopy, exogenous administration of CXCL9/10 was sufficient to correct sepsis-induced impairments in recruitment of effector cells at the localized site of T(RM) antigen recognition. Thus, sepsis has the capacity to alter skin T(RM) anamnestic responses without directly impacting T(RM) number and/or function, an observation that helps to further define the immunoparalysis phase in sepsis survivors.
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spelling pubmed-55990542017-09-22 Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells Danahy, Derek B. Anthony, Scott M. Jensen, Isaac J. Hartwig, Stacey M. Shan, Qiang Xue, Hai-Hui Harty, John T. Griffith, Thomas S. Badovinac, Vladimir P. PLoS Pathog Research Article Sepsis is a systemic infection that enhances host vulnerability to secondary infections normally controlled by T cells. Using CLP sepsis model, we observed that sepsis induces apoptosis of circulating memory CD8 T-cells (T(CIRCM)) and diminishes their effector functions, leading to impaired CD8 T-cell mediated protection to systemic pathogen re-infection. In the context of localized re-infections, tissue resident memory CD8 T-cells (T(RM)) provide robust protection in a variety of infectious models. T(RM) rapidly ‘sense’ infection in non-lymphoid tissues and ‘alarm’ the host by enhancing immune cell recruitment to the site of the infection to accelerate pathogen clearance. Here, we show that compared to pathogen-specific T(CIRCM), sepsis does not invoke significant numerical decline of Vaccinia virus induced skin-T(RM) keeping their effector functions (e.g., Ag-dependent IFN-γ production) intact. IFN-γ-mediated recruitment of immune cells to the site of localized infection was, however, reduced in CLP hosts despite T(RM) maintaining their ‘sensing and alarming’ functions. The capacity of memory CD8 T-cells in the septic environment to respond to inflammatory cues and arrive to the site of secondary infection/antigen exposure remained normal suggesting T-cell-extrinsic factors contributed to the observed lesion. Mechanistically, we showed that IFN-γ produced rapidly during sepsis-induced cytokine storm leads to reduced IFN-γR1 expression on vascular endothelium. As a consequence, decreased expression of adhesion molecules and/or chemokines (VCAM1 and CXCL9) on skin endothelial cells in response to T(RM)-derived IFN-γ was observed, leading to sub-optimal bystander-recruitment of effector cells and increased susceptibility to pathogen re-encounter. Importantly, as visualized by intravital 2-photon microscopy, exogenous administration of CXCL9/10 was sufficient to correct sepsis-induced impairments in recruitment of effector cells at the localized site of T(RM) antigen recognition. Thus, sepsis has the capacity to alter skin T(RM) anamnestic responses without directly impacting T(RM) number and/or function, an observation that helps to further define the immunoparalysis phase in sepsis survivors. Public Library of Science 2017-09-14 /pmc/articles/PMC5599054/ /pubmed/28910403 http://dx.doi.org/10.1371/journal.ppat.1006569 Text en https://creativecommons.org/publicdomain/zero/1.0/ This is an open access article, free of all copyright, and may be freely reproduced, distributed, transmitted, modified, built upon, or otherwise used by anyone for any lawful purpose. The work is made available under the Creative Commons CC0 (https://creativecommons.org/publicdomain/zero/1.0/) public domain dedication.
spellingShingle Research Article
Danahy, Derek B.
Anthony, Scott M.
Jensen, Isaac J.
Hartwig, Stacey M.
Shan, Qiang
Xue, Hai-Hui
Harty, John T.
Griffith, Thomas S.
Badovinac, Vladimir P.
Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells
title Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells
title_full Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells
title_fullStr Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells
title_full_unstemmed Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells
title_short Polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory CD8 T cells
title_sort polymicrobial sepsis impairs bystander recruitment of effector cells to infected skin despite optimal sensing and alarming function of skin resident memory cd8 t cells
topic Research Article
url https://www.ncbi.nlm.nih.gov/pmc/articles/PMC5599054/
https://www.ncbi.nlm.nih.gov/pubmed/28910403
http://dx.doi.org/10.1371/journal.ppat.1006569
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