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IL-33 promotes type 1 cytokine expression via p38 MAPK in human NK cells

David E. Ochayon, Ayad Ali, Pablo C. Alarcon, Durga Krishnamurthy, Leah C. Kottyan, Michael T. Borchers, Stephen N. Waggoner

2020Journal of Leukocyte Biology52 citationsDOIOpen Access PDF

Abstract

This study tests the hypothesis that activation of MAPK by physiologically relevant concentrations of IL-33 contributes to enhanced cytokine expression by IL-12 stimulated human NK cells. While IL-33 canonically triggers type 2 cytokine responses, this cytokine can also synergize with type 1 cytokines like IL-12 to provoke IFN-γ. We show that picogram concentrations of IL-12 and IL-33 are sufficient to promote robust secretion of IFN-γ by human NK cells that greatly exceeds resposes to either cytokine alone. Nanogram doses of IL-33, potentially consistent with levels in tissue microenvironments, synergize with IL-12 to induce secretion of additional cytokines, including TNF and GM-CSF. IL-33-induced activation of the p38 MAPK pathway in human NK cells is crucial for enhanced release of IFN-γ and TNF in response to IL-12. Mechanistically, IL-33-induced p38 MAPK signaling enhances stability of IFNG transcripts and triggers A disintegrin and metalloproteinase domain 17 (ADAM17) mediated cleavage of TNF from the cell surface. These data support our hypothesis and suggest that altered sensitivity of NK cells to IL-12 in the presence of IL-33 may have important consequences in diseases associated with mixed cytokine milieus, like asthma and chronic obstructive pulmonary disease.

Topics & Concepts

CytokineBiologySecretionp38 mitogen-activated protein kinasesTumor necrosis factor alphaCell biologyMAPK/ERK pathwayImmunologySignal transductionEndocrinologyIL-33, ST2, and ILC PathwaysEosinophilic EsophagitisImmune Cell Function and Interaction
IL-33 promotes type 1 cytokine expression via p38 MAPK in human NK cells | Litcius