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首页> 外文OA文献 >Alcohol-induced IL-1beta in the brain is mediated by NLRP3/ASC inflammasome activation that amplifies neuroinflammation
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Alcohol-induced IL-1beta in the brain is mediated by NLRP3/ASC inflammasome activation that amplifies neuroinflammation

机译:大脑中酒精诱导的IL-1β由NLRp3 / asC炎性体激活介导,可激活神经炎症

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Alcohol-induced neuroinflammation is mediated by proinflammatory cytokines, including IL-1beta. IL-1beta production requires caspase-1 activation by inflammasomes-multiprotein complexes that are assembled in response to danger signals. We hypothesized that alcohol-induced inflammasome activation contributes to increased IL-1beta in the brain. WT and TLR4-, NLRP3-, and ASC-deficient (KO) mice received an ethanol-containing or isocaloric control diet for 5 weeks, and some received the rIL-1ra, anakinra, or saline treatment. Inflammasome activation, proinflammatory cytokines, endotoxin, and HMGB1 were measured in the cerebellum. Expression of inflammasome components (NLRP1, NLRP3, ASC) and proinflammatory cytokines (TNF-alpha, MCP-1) was increased in brains of alcohol-fed compared with control mice. Increased caspase-1 activity and IL-1beta protein in ethanol-fed mice indicated inflammasome activation. TLR4 deficiency protected from TNF-alpha, MCP-1, and attenuated alcohol-induced IL-1beta increases. The TLR4 ligand, LPS, was not increased in the cerebellum. However, we found up-regulation of acetylated and phosphorylated HMGB1 and increased expression of the HMGB1 receptors (TLR2, TLR4, TLR9, RAGE) in alcohol-fed mice. NLRP3- or ASC-deficient mice were protected from caspase-1 activation and alcohol-induced IL-1beta increase in the brain. Furthermore, in vivo treatment with rIL-1ra prevented alcohol-induced inflammasome activation and IL-1beta, TNF-alpha, and acetylated HMGB1 increases in the cerebellum. Conversely, intracranial IL-1beta administration induced TNF-alpha and MCP-1 in the cerebellum. In conclusion, alcohol up-regulates and activates the NLRP3/ASC inflammasome, leading to caspase-1 activation and IL-1beta increase in the cerebellum. IL-1beta amplifies neuroinflammation, and disruption of IL-1/IL-1R signaling prevents alcohol-induced inflammasome activation and neuroinflammation. Increased levels of acetylated and phosphorylated HMGB1 may contribute to alcoholic neuroinflammation.
机译:酒精诱导的神经炎症是由包括IL-1β在内的促炎细胞因子介导的。 IL-1beta的产生需要通过响应危险信号而组装的炎症小体-多蛋白复合物激活caspase-1。我们假设酒精诱导的炎症小体激活导致大脑中IL-1beta升高。 WT和TLR4-,NLRP3-和ASC缺陷(KO)小鼠接受了含乙醇或等热量的对照饮食5周,其中一些接受了rIL-1ra,anakinra或盐水治疗。在小脑中测量炎症小体激活,促炎细胞因子,内毒素和HMGB1。与对照组相比,酒精喂养的大脑中炎症小体成分(NLRP1,NLRP3,ASC)和促炎细胞因子(TNF-α,MCP-1)的表达增加。在用乙醇喂养的小鼠中,caspase-1活性和IL-1beta蛋白升高表明炎症小体活化。 TLR4缺乏保护免受TNF-α,MCP-1和减弱的酒精诱导的IL-1beta的影响。 TLR4配体LPS在小脑中没有增加。但是,我们发现在酒精喂养的小鼠中,乙酰化和磷酸化的HMGB1上调并增加了HMGB1受体(TLR2,TLR4,TLR9,RAGE)的表达。 NLRP3或ASC缺陷小鼠受到caspase-1激活和酒精诱导的脑内IL-1beta升高的保护。此外,在体内用rIL-1ra治疗可防止酒精诱导的炎症小体活化,并且小脑中IL-1beta,TNF-α和乙酰化HMGB1升高。相反,颅内IL-1β给药可诱导小脑中的TNF-α和MCP-1。总之,酒精会上调并激活NLRP3 / ASC炎性体,导致小脑中caspase-1激活和IL-1beta升高。 IL-1β放大了神经炎症,IL-1 / IL-1R信号传导的破坏阻止了酒精引起的炎症小体活化和神经炎症。乙酰化和磷酸化的HMGB1水平升高可能会导致酒精性神经炎症。

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