Author: Nizami, Sohaib; Arunasalam, Kanisa; Green, Jack; Cook, James; Lawrence, Catherine B.; Zarganesâ€Tzitzikas, Tryfon; Davis, John B.; Di Daniel, Elena; Brough, David
Title: Inhibition of the NLRP3 inflammasome by HSP90 inhibitors Cord-id: feqja60i Document date: 2020_10_30
ID: feqja60i
Snippet: Excessive and dysregulated inflammation is known to contribute to disease progression. HSP90 is an intracellular chaperone known to regulate inflammatory processes including the NLRP3 inflammasome and secretion of the proâ€inflammatory cytokine interleukin(IL)â€1β. Here, primarily using an in vitro inflammasome ASC speck assay, and an in vivo model of murine peritonitis, we tested the utility of HSP90 inhibitors as antiâ€inflammatory molecules. We report that the HSP90 inhibitor EC144 effect
Document: Excessive and dysregulated inflammation is known to contribute to disease progression. HSP90 is an intracellular chaperone known to regulate inflammatory processes including the NLRP3 inflammasome and secretion of the proâ€inflammatory cytokine interleukin(IL)â€1β. Here, primarily using an in vitro inflammasome ASC speck assay, and an in vivo model of murine peritonitis, we tested the utility of HSP90 inhibitors as antiâ€inflammatory molecules. We report that the HSP90 inhibitor EC144 effectively inhibited inflammatory processes including priming and activation of NLRP3 in vitro and in vivo. A specific inhibitor of the β HSP90 isoform was ineffective suggesting the importance of the α isoform in inflammatory signalling. EC144 inhibited ILâ€1β and ILâ€6 in vivo when administered orally, and was brainâ€penetrant. These data suggest that HSP90 inhibitors may be useful for targeting inflammation in diverse diseases that are worsened by the presence of inflammation.
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