前沿:热休克蛋白 gp96 在 APC 中激活炎症小体信号平台。
Cutting Edge: The Heat Shock Protein gp96 Activates Inflammasome-Signaling Platforms in APCs.
机构信息
School of Medicine, Tsinghua University, Beijing 100084, China.
Department of Immunology, University of Pittsburgh, Pittsburgh, PA 15261.
出版信息
J Immunol. 2018 Oct 15;201(8):2209-2214. doi: 10.4049/jimmunol.1800505. Epub 2018 Sep 12.
Abstract
Several heat shock proteins (HSPs) prime immune responses, which are, in part, a result of activation of APCs. APCs respond to these immunogenic HSPs by upregulating costimulatory molecules and secreting cytokines, including IL-1β. These HSP-mediated responses are central mediators in pathological conditions ranging from cancer, sterile inflammation associated with trauma, and rheumatoid arthritis. We tested in this study the requirement of inflammasomes in the release of IL-1β by one immunogenic HSP, gp96. Our results show that murine APCs activate NLRP3 inflammasomes in response to gp96 by K efflux. This is shown to initiate inflammatory conditions in vivo in the absence of additional known inflammasome activators or infection. These results document a novel mechanism by which proteins of endogenous origin, the HSPs, can modulate an inflammatory response following their release from aberrant cells.
摘要
几种热休克蛋白(HSPs)引发免疫反应,部分原因是 APCs 的激活。APC 对这些免疫原性 HSP 的反应是上调共刺激分子并分泌细胞因子,包括 IL-1β。这些 HSP 介导的反应是从癌症、创伤相关的无菌炎症到类风湿关节炎等病理状况的中心介质。在这项研究中,我们测试了炎症小体在一种免疫原性 HSP,gp96 释放 IL-1β 中的作用。我们的结果表明,鼠 APCs 通过 K+外排对 gp96 激活 NLRP3 炎症小体。这表明在没有其他已知的炎症小体激活剂或感染的情况下,体内会引发炎症状态。这些结果记录了内源性蛋白 HSP 可以在从异常细胞释放后通过调节炎症反应的一种新机制。
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