IL-10 Restricts Activation-Induced Death of NK Cells during Acute Murine Cytomegalovirus Infection

Stacey, Maria A.; Marsden, Morgan; Wang, Edward Chung Yern; Wilkinson, Gavin William Grahame; Humphreys, Ian R.

doi:10.4049/jimmunol.1101021

Cited by 45 publications

(50 citation statements)

References 58 publications

(71 reference statements)

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“…Of note, NK depletion did not influence neutrophil accumulation in infected tissues (data not shown). Taken with the observations that T cells secrete IL-22 (Figures 2A–2C) and that MCMV replication (which is elevated after NK1.1 depletion in this model [Stacey et al., 2011]) directly induces CXCL1 production (Figure 3J), these results demonstrate that NK1.1 − cells are capable of promoting neutrophil recruitment in the absence of NK cells. Importantly, these results also imply that neutrophil activation of NK cells is not the primary mechanism through which neutrophils control MCMV.…”

Section: Resultssupporting

confidence: 90%

Neutrophils Recruited by IL-22 in Peripheral Tissues Function as TRAIL-Dependent Antiviral Effectors against MCMV

Stacey

Marsden

et al. 2014

Cell Host & Microbe

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SummaryDuring primary infection, murine cytomegalovirus (MCMV) spreads systemically, resulting in virus replication and pathology in multiple organs. This disseminated infection is ultimately controlled, but the underlying immune defense mechanisms are unclear. Investigating the role of the cytokine IL-22 in MCMV infection, we discovered an unanticipated function for neutrophils as potent antiviral effector cells that restrict viral replication and associated pathogenesis in peripheral organs. NK-, NKT-, and T cell-secreted IL-22 orchestrated antiviral neutrophil-mediated responses via induction in stromal nonhematopoietic tissue of the neutrophil-recruiting chemokine CXCL1. The antiviral effector properties of infiltrating neutrophils were directly linked to the expression of TNF-related apoptosis-inducing ligand (TRAIL). Our data identify a role for neutrophils in antiviral defense, and establish a functional link between IL-22 and the control of antiviral neutrophil responses that prevents pathogenic herpesvirus infection in peripheral organs.

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Section: Resultssupporting

confidence: 90%

Neutrophils Recruited by IL-22 in Peripheral Tissues Function as TRAIL-Dependent Antiviral Effectors against MCMV

Stacey

Marsden

et al. 2014

Cell Host & Microbe

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“…4B). In line with previously published data 27 and with the notion that high expression of the activation marker CD25 is per se associated with increased AnnexinV binding, 28 we attribute the extensive rate of apoptosis in CIML-NK cells to the induction of an IL12-mediated "activationinduced cell death" (AICD). As a result of this apparently shifted cell balance between proliferation and apoptosis the total cell number of TIML-NK cells was upregulated (d3: fold increase 1.53 § 0.47, proliferation >> apoptosis) but virtually unchanged in CIML-NK cells (d3: fold increase 1.0 § 0.25, proliferation D apoptosis) (Fig.…”

Section: Cd3supporting

confidence: 76%

Tumor-priming converts NK cells to memory-like NK cells

et al. 2017

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Fascinating earlier evidence suggests an intrinsic capacity of human natural killer (NK) cells to acquire adaptive immune features in the context of cytomegalovirus (CMV) infection or pro-inflammatory cytokine stimulation. Since the role of memory NK cells in cancer has so far remained elusive and adoptive NK cell transfer in relapsing pediatric acute B cell precursor leukemia (BCP-ALL) patients awaits improvement, we asked the question whether tumor-priming could promote the generation of memory NK cells with enhanced graft-vs.-leukemia (GvL) reactivity. Here, we provide substantial evidence that priming of naive human NK cells with pediatric acute B cell leukemia or acute myeloid leukemia specimens induces a functional conversion to tumor-induced memory-like (TIML)-NK cells displaying a heightened tumorspecific cytotoxicity and enhanced perforin synthesis. Cell cycles analyses reveal that tumor-priming sustainably alters the balance between NK cell activation and apoptosis in favor of survival. In addition, gene expression patterns differ between TIML-and cytokine-induced memory-like (CIML)-NK cells with the magnitude of regulated genes being distinctly higher in TIML-NK cells. As such, the tumor-induced conversion of NK cells triggers the emergence of a so far unacknowledged NK cell differentiation stage that might promote GvL effects in the context of adoptive cell transfer.

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“…Leukocytes were extracted from murine spleen, salivary glands and lungs as described previously [13,60]. For CD4 + functional responses, isolated leukocytes were stimulated for 2 hours with 3 μg/ml m09, (GYLYIYPSAGNSFDL), M25 (NHLYETPISATAMVI), m139 (TRPYRYPRVCDASLS), and m142 (RSRYLTAAAVTAVLQ) MCMV MHCII peptides (Genscript).…”

Section: Methodsmentioning

confidence: 99%

“…Data obtained from the MCMV model has demonstrated an important protective role for cellular IL-10 during acute CMV infection. Myeloid cells and B cells are the predominant sources of IL-10 during initial MCMV infection [13,14]. IL-10 limits virus induced weight loss, pro-inflammatory cytokine production and activation-induced NK cell death [13–15].…”

Section: Introductionmentioning

confidence: 99%

“…Myeloid cells and B cells are the predominant sources of IL-10 during initial MCMV infection [13,14]. IL-10 limits virus induced weight loss, pro-inflammatory cytokine production and activation-induced NK cell death [13–15]. Sustained acute MCMV replication in situations of high virus load also induces IL-10 production by NK cells that restricts CD8 + T cell-mediated immune pathology [16].…”

Section: Introductionmentioning

confidence: 99%

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Cytomegalovirus-Specific IL-10-Producing CD4+ T Cells Are Governed by Type-I IFN-Induced IL-27 and Promote Virus Persistence

et al. 2016

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CD4+ T cells support host defence against herpesviruses and other viral pathogens. We identified that CD4+ T cells from systemic and mucosal tissues of hosts infected with the β-herpesviridae human cytomegalovirus (HCMV) or murine cytomegalovirus (MCMV) express the regulatory cytokine interleukin (IL)-10. IL-10+CD4+ T cells co-expressed TH1-associated transcription factors and chemokine receptors. Mice lacking T cell-derived IL-10 elicited enhanced antiviral T cell responses and restricted MCMV persistence in salivary glands and secretion in saliva. Thus, IL-10+CD4+ T cells suppress antiviral immune responses against CMV. Expansion of this T-cell population in the periphery was promoted by IL-27 whereas mucosal IL-10+ T cell responses were ICOS-dependent. Infected Il27rα-deficient mice with reduced peripheral IL-10+CD4+ T cell accumulation displayed robust T cell responses and restricted MCMV persistence and shedding. Temporal inhibition experiments revealed that IL-27R signaling during initial infection was required for the suppression of T cell immunity and control of virus shedding during MCMV persistence. IL-27 production was promoted by type-I IFN, suggesting that β-herpesviridae exploit the immune-regulatory properties of this antiviral pathway to establish chronicity. Further, our data reveal that cytokine signaling events during initial infection profoundly influence virus chronicity.

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IL-10 Restricts Activation-Induced Death of NK Cells during Acute Murine Cytomegalovirus Infection

Cited by 45 publications

References 58 publications

Neutrophils Recruited by IL-22 in Peripheral Tissues Function as TRAIL-Dependent Antiviral Effectors against MCMV

Neutrophils Recruited by IL-22 in Peripheral Tissues Function as TRAIL-Dependent Antiviral Effectors against MCMV

Tumor-priming converts NK cells to memory-like NK cells

Cytomegalovirus-Specific IL-10-Producing CD4+ T Cells Are Governed by Type-I IFN-Induced IL-27 and Promote Virus Persistence

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