| Literature DB >> 30089254 |
Mercedes Monteleone1, Amanda C Stanley1, Kaiwen W Chen1, Darren L Brown1, Jelena S Bezbradica1, Jessica B von Pein1, Caroline L Holley1, Dave Boucher1, Melanie R Shakespear1, Ronan Kapetanovic1, Verena Rolfes1, Matthew J Sweet1, Jennifer L Stow1, Kate Schroder2.
Abstract
IL-1β requires processing by caspase-1 to generate the active, pro-inflammatory cytokine. Acute IL-1β secretion from inflammasome-activated macrophages requires caspase-1-dependent GSDMD cleavage, which also induces pyroptosis. Mechanisms of IL-1β secretion by pyroptotic and non-pyroptotic cells, and the precise functions of caspase-1 and GSDMD therein, are unresolved. Here, we show that, while efficient early secretion of endogenous IL-1β from primary non-pyroptotic myeloid cells in vitro requires GSDMD, later IL-1β release in vitro and in vivo proceeds independently of GSDMD. IL-1β maturation is sufficient for slow, caspase-1/GSDMD-independent secretion of ectopic IL-1β from resting, non-pyroptotic macrophages, but the speed of IL-1β release is boosted by inflammasome activation, via caspase-1 and GSDMD. IL-1β cleavage induces IL-1β enrichment at PIP2-enriched plasma membrane ruffles, and this is a prerequisite for IL-1β secretion and is mediated by a polybasic motif within the cytokine. We thus reveal a mechanism in which maturation-induced IL-1β trafficking facilitates its unconventional secretion.Entities:
Keywords: caspase-1; gasdermin; inflammasome; interleukin-1; macrophage; neutrophil; phosphoinositides; pyroptosis; trafficking; unconventional protein secretion
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Year: 2018 PMID: 30089254 DOI: 10.1016/j.celrep.2018.07.027
Source DB: PubMed Journal: Cell Rep Impact factor: 9.423