Polymicrobial Sepsis Impairs Antigen-Specific Memory CD4 T Cell-Mediated Immunity

Sjaastad, Frances V.; Kucaba, Tamara A.; Dileepan, Thamotharampillai; Swanson, Whitney; Dail, Cody; Cabrera-Pérez, Javier; Murphy, Katherine A.; Badovinac, Vladimir P.; Griffith, Thomas S.

doi:10.3389/fimmu.2020.01786

Cited by 20 publications

(13 citation statements)

References 87 publications

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“…It is well-documented that sepsis leads to impaired adaptive immune responses, including reduced Ag-specific humoral responses (20)(21)(22). B and T cell defects have been demonstrated in sepsis mice (21)(22)(23), but there are some less well-examined cell types, including FDCs, the dysfunction of which may also contribute to the overall defect. Some reports show that FDCs undergo apoptosis at the onset of sepsis through a caspase-3-mediated mechanism (24,25).…”

Section: Introductionmentioning

confidence: 99%

Follicular dendritic cell dysfunction contributes to impaired antigen-specific humoral responses in sepsis-surviving mice

Rana¹,

Bella²,

Lederman³

et al. 2021

Journal of Clinical Investigation

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Section: Introductionmentioning

confidence: 99%

Follicular dendritic cell dysfunction contributes to impaired antigen-specific humoral responses in sepsis-surviving mice

Rana¹,

Bella²,

Lederman³

et al. 2021

Journal of Clinical Investigation

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“…These profound impairments are sufficient to reduce the 5 year survival of septic cohorts, relative to non-septic cohorts; consequently, the majority of sepsis-associated mortality is late mortality secondary to the cytokine storm ( Dombrovskiy et al, 2007 ; Donnelly et al, 2015 ; Gaieski et al, 2013 ). This immunologic impairment is typified by transient lymphopenia and reduced capacity of various surviving lymphocyte populations to perform effector function ( Hotchkiss et al, 2016 ; Hotchkiss et al, 2013 ), including CD4 ( Cabrera-Perez et al, 2014 ; Cabrera-Perez et al, 2015 ; Chen et al, 2017 ; Jensen et al, 2020 ; Martin et al, 2020 ; Sjaastad et al, 2020b ) and CD8 T cells ( Condotta et al, 2013 ; Danahy et al, 2017 ; Danahy et al, 2019 ; Duong et al, 2014 ; Serbanescu et al, 2016 ; Xie et al, 2019 ), B cells ( Hotchkiss et al, 2001 ; Sjaastad et al, 2018 ; Unsinger et al, 2010 ), NK cells ( Hou et al, 2014 ; Jensen et al, 2021b ; Jensen et al, 2018b ; Souza-Fonseca-Guimaraes et al, 2012 ), and dendritic cells (DCs) ( Poehlmann et al, 2009 ; Roquilly et al, 2017 ; Strother et al, 2016 ). We and others have characterized numerous impairments early after sepsis induction; however, the extent to which those cell populations recover in number and function remains largely unknown.…”

Section: Introductionmentioning

confidence: 99%

Sepsis leads to lasting changes in phenotype and function of memory CD8 T cells

Jensen

McGonagill

et al. 2021

eLife

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The global health burden due to sepsis and the associated cytokine storm is substantial. While early intervention has improved survival during the cytokine storm, those that survive can enter a state of chronic immunoparalysis defined by transient lymphopenia and functional deficits of surviving cells. Memory CD8 T cells provide rapid cytolysis and cytokine production following re-encounter with their cognate antigen to promote long-term immunity, and CD8 T cell impairment due to sepsis can pre-dispose individuals to re-infection. While the acute influence of sepsis on memory CD8 T cells has been characterized, if and to what extent pre-existing memory CD8 T cells recover remains unknown. Here, we observed that central memory CD8 T cells (TCM) from septic patients proliferate more than those from healthy individuals. Utilizing LCMV immune mice and a CLP model to induce sepsis, we demonstrated that TCM proliferation is associated with numerical recovery of pathogen-specific memory CD8 T cells following sepsis-induced lymphopenia. This increased proliferation leads to changes in composition of memory CD8 T cell compartment and altered tissue localization. Further, memory CD8 T cells from sepsis survivors have an altered transcriptional profile and chromatin accessibility indicating long-lasting T cell intrinsic changes. The sepsis-induced changes in the composition of the memory CD8 T cell pool and transcriptional landscape culminated in altered T cell function and reduced capacity to control L. monocytogenes infection. Thus, sepsis leads to long-term alterations in memory CD8 T cell phenotype, protective function and localization potentially changing host capacity to respond to re-infection.

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“…While there is a dearth of knowledge regarding the impact of sepsis on autoimmunity, descriptions of how sepsis influences specific cell subsets can provide insight into how autoimmune disease may be influenced. With regard to the critical role for CD4 T cells in EAE disease, the sepsis-induced lymphopenic state is known to impact both naive and memory CD4 T cells ( Cabrera-Perez et al, 2016 ; Cabrera-Perez et al, 2015 ; Chen et al, 2017 ; Jensen et al, 2018a ; Sjaastad et al, 2020b ). In particular, sepsis can diminish the number of naive CD4 T cell precursors subsequently limiting the number of cells capable of responding to a given antigen ( Cabrera-Perez et al, 2015 ; Martin et al, 2020 ).…”

Section: Introductionmentioning

confidence: 99%

Sepsis impedes EAE disease development and diminishes autoantigen-specific naive CD4 T cells

Jensen

Sjaastad

et al. 2020

eLife

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Evaluation of sepsis-induced immunoparalysis has highlighted how decreased lymphocyte number/function contribute to worsened infection/cancer. Yet an interesting contrast exists with autoimmune disease development, wherein diminishing pathogenic effectors may benefit the post-septic host. Within this framework the impact of cecal ligation and puncture (CLP)-induced sepsis on the development of experimental autoimmune encephalomyelitis (EAE) was explored. Notably, CLP mice have delayed onset and reduced disease severity, relative to sham mice. Reduction in disease severity was associated with reduced number, but not function, of autoantigen (MOG)-specific pathogenic CD4 T cells in the CNS during disease and draining lymph node during priming. Numerical deficits of CD4 T cell effectors are associated with the loss of MOG-specific naive precursors. Critically, transfer of MOG-TCR transgenic (2D2) CD4 T cells after, but not before, CLP led to EAE disease equivalent to sham mice. Thus, broad impairment of antigenic responses, including autoantigens, is a hallmark of sepsis-induced immunoparalysis.

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Polymicrobial Sepsis Impairs Antigen-Specific Memory CD4 T Cell-Mediated Immunity

Cited by 20 publications

References 87 publications

Follicular dendritic cell dysfunction contributes to impaired antigen-specific humoral responses in sepsis-surviving mice

Follicular dendritic cell dysfunction contributes to impaired antigen-specific humoral responses in sepsis-surviving mice

Sepsis leads to lasting changes in phenotype and function of memory CD8 T cells

Sepsis impedes EAE disease development and diminishes autoantigen-specific naive CD4 T cells

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