Severe Lymphopenia Is Associated with Elevated Plasma Interleukin-15 Levels and Increased Mortality During Severe Sepsis

Chung, Kuei-Pin; Chang, Hao-Chieh; Lo, Su Shun; Chang, Li-Chien; Lin, Shu-Yung; Cheng, Aristine; Huang, Yen‐Tsung; Chen, Chih‐Cheng; Lee, Meng-Rui; Chen, Yi-Jung; Hou, Hsin‐Han; Hsu, Chia-Lin; Jerng, Jih-Shuin; Ho, Chao‐Chi; Huang, Ming‐Bao; Yu, Chong‐Jen; Yang, Pan‐Chyr

doi:10.1097/shk.0000000000000347

Cited by 67 publications

(61 citation statements)

References 31 publications

(41 reference statements)

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“…Given that sepsis is generally accompanied by acute lymphopenia (17,52,53), these findings suggested that sepsis survivors replenish the hole created in their T cell compartment. Several studies reported an association between T cell numbers and prognosis of sepsis patients beyond the acute disease phase (17,54,55), leading to the proposal that persistent lymphopenia could serve as a biomarker for late mortality in sepsis (17,55). In principle, the absence of lymphopenia in the present patient cohort is in agreement with that notion, given that all 12 patients were alive at the 28-d follow-up upon discharge from the postacute care hospital (Table II).…”

Section: Discussionsupporting

confidence: 80%

“…Another factor that is likely to persistently affect the adaptive immune system of the sepsis patient is the contraction of the T cell clonal repertoire as a consequence of early apoptotic T cell loss. As argued previously (17,22,55), the irreversible loss of T cell clones during early sepsis causes a contraction of the T cell repertoire that can compromise the ability of the host to react to ensuing infections. According to that scenario, "prosurvival" cytokines, such as IL-7 or IL-15, which prevent early T cell apoptosis and show high efficacy in rodent models of sepsis (13,56,73), are promising therapeutics that are already being tested in the clinic.…”

Section: Discussionmentioning

confidence: 84%

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Chronic Critical Illness from Sepsis Is Associated with an Enhanced TCR Response

Borken

Markwart

Requardt

et al. 2017

The Journal of Immunology

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Sepsis is characterized by a disproportionate host response to infection that often culminates in multiple organ failure. Current concepts invoke a deregulated immune reaction involving features of hyperinflammation, as well as protracted immune suppression. However, owing to the scarcity of human data, the precise origin of a long-term suppression of adaptive immunity remains doubtful. We report on an explorative clinical study of chronic critical illness (CCI) patients aimed at assessing the long-term consequences of sepsis on T cell function. Blood was drawn from 12 male CCI patients (median age 67 y, range 48-79 y) receiving continuous mechanical ventilation and renal replacement therapy in a long-term care hospital who had been treated in an external acute care hospital for severe sepsis. T cells were purified and subjected to flow cytometric immune-phenotyping and functional assays. We found that T cells from CCI patients featured higher basal levels of activation and stronger expression of the inhibitory surface receptor programmed cell death 1 compared with controls. However, T cells from CCI patients exhibited no suppressed TCR response at the level of proximal TCR signaling (activation/phosphorylation of PLCγ, Erk, Akt, LAT), activation marker upregulation (CD69, CD25, CD154, NUR77), IL-2 production, or clonal expansion. Rather, our data illustrate an augmented response in T cells from CCI patients in response to TCR/coreceptor (CD3/CD28) challenge. Thus, the present findings reveal that CCI sepsis patients feature signs of immune suppression but that their T cells exhibit a primed, rather than a suppressed, phenotype in their TCR response, arguing against a generalized T cell paralysis as a major cause of protracted immune suppression from sepsis.

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Section: Discussionsupporting

confidence: 80%

Section: Discussionmentioning

confidence: 84%

Chronic Critical Illness from Sepsis Is Associated with an Enhanced TCR Response

Borken

Markwart

Requardt

et al. 2017

The Journal of Immunology

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“…In sepsis, IL-15 blocked the apoptosis of CD8 + T cells and increased the abundance of Bcl-2 while decreasing Bim and Puma (343). However, patients with sepsis with severe lymphopenia had downregulated Bcl-2 mRNA expression in peripheral blood mononuclear cells, despite increased plasma IL-15 concentrations (344). Thus, further studies are needed to understand the potential role of IL-15 in sepsis.…”

Section: Maintaining T Cell Survival For Therapeutic Purposementioning

confidence: 99%

Dying to protect: cell death and the control of T‐cell homeostasis

Shanmuganad

Carroll

et al. 2017

Immunological Reviews

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Summary T cells play a critical role in immune responses as they specifically recognize peptide/MHC complexes with their T cell receptors (TCRs) and initiate adaptive immune responses. While T cells are critical for performing appropriate effector functions and maintaining immune memory, they also can cause autoimmunity or neoplasia if misdirected or dysregulated. Thus, T cells must be tightly regulated from their development onward. Maintenance of appropriate T cell homeostasis is essential to promote protective immunity and limit autoimmunity and neoplasia. This review will focus on the role of cell death in maintenance of T cell homeostasis and outline novel therapeutic strategies tailored to manipulate cell death to limit T cell survival (eg autoimmunity and transplantation) or enhance T cell survival (eg vaccination, immune-deficiency).

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“…Every lymphocyte subpopulation was affected (except regulatory T cells, see below). Most importantly, the extent of this lymphopenia has been shown to correlate with the development of HAI and/or death at 28 days . Importantly, this lymphopenia may last for several weeks after the onset of sepsis and this lack of recovery was associated with delayed infectious complications .…”

Section: Lymphocytesmentioning

confidence: 99%

Sepsis‐induced immune alterations monitoring by flow cytometry as a promising tool for individualized therapy

Monneret

Venet

2015

Cytometry Part B Clinical

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Septic syndromes remain a major although largely under-recognized health care problem and represent the first cause of mortality in intensive care units. While sepsis has, for long, been solely described as inducing a tremendous systemic inflammatory response, novel findings indicate that sepsis indeed initiates a more complex immunologic response that varies over time, with the concomitant occurrence of both pro-and anti-inflammatory mechanisms. As a resultant, after a short proinflammatory phase, septic patients enter a stage of protracted immunosuppression. This is illustrated in those patients by reactivation of dormant viruses (CMV or HSV) or infections due to pathogens, including fungi, which are normally pathogenic solely in immunocompromised hosts. Although mechanisms are not totally understood, these alterations might be directly responsible for worsening outcome in patients who survived initial resuscitation as nearly all immune functions are deeply compromised. Indeed, the magnitude and persistence over time of these dysfunctions have been associated with increased mortality and health-care associated infection rate. Consequently, new promising therapeutic avenues are currently emerging from those recent findings such as adjunctive immunostimulation (IFN-g, GM-CSF, IL-7, anti-PD1/L1 antibodies) for the most immunosuppressed patients. Nevertheless, as there is no clinical sign of immune dysfunctions, the prerequisite for such therapeutic intervention relies on our capacity in identifying the patients who could benefit from immunostimulation. To date, the most robust biomarkers of sepsis-induced immunosuppression are measured by flow cytometry. Of them, the decreased expression of monocyte HLA-DR appears as a "gold standard." This review reports on the mechanisms sustaining sepsis-induced immunosuppression and its related biomarkers measurable by flow cytometry. The objective is to integrate the most recent facts in an up-to-date account of clinical results, flow cytometry aspects as well as issues in results standardization for multicenter studies. V C 2015 International Clinical Cytometry Society

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Severe Lymphopenia Is Associated with Elevated Plasma Interleukin-15 Levels and Increased Mortality During Severe Sepsis

Cited by 67 publications

References 31 publications

Chronic Critical Illness from Sepsis Is Associated with an Enhanced TCR Response

Chronic Critical Illness from Sepsis Is Associated with an Enhanced TCR Response

Dying to protect: cell death and the control of T‐cell homeostasis

Sepsis‐induced immune alterations monitoring by flow cytometry as a promising tool for individualized therapy

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