Rosmarinic acid inhibits nicotine-induced C-reactive protein generation by inhibiting NLRP3 inflammasome activation in smooth muscle cells

Atherosclerosis is widely known to be a chronic inflammatory disease. C-reactive protein (CRP), an important inflammatory factor, plays an essential role in the pathogenesis of atherosclerosis. Nicotine, the main addictive component of cigarette, has been shown to induce the production of CRP. The aim of this study was to investigate the effect of rosmarinic acid (RA), a polyphenol with antiinflammatory activity, on nicotine-induced elevation of CRP in vascular smooth muscle cells (VSMCs). We found that pretreatment of VSMCs with RA attenuated nicotine-induced expression of CRP in a time- and dose-dependant manner. In addition, RA also inhibited the activation of NLR family pyrin domain containing 3 (NLRP3) inflammasome and reactive oxygen species (ROS) production resulting from nicotine treatment in VSMCs. To confirm these findings in vivo, we constructed a nicotine-induced atherosclerosis rat model. RA did not significantly reduce the serum nicotine level of the rats, whereas it significantly decreased the levels of serum lipids, including concentrations of cholesterol, triglycerides, and low-density lipoprotein cholesterol, and the serum level of CRP. RA also led to diminished nicotine-induced activation of NLRP3 inflammasome and elevation in the CRP level in the aortic tissue of the model rats. The results of this study suggested a protective role of RA in nicotine-induced atherosclerosis by inhibiting the ROS–NLRP3 inflammasome–CRP axial, and RA therefore represented a potential effective therapeutic approach to atherosclerosis, in particular for those who smoke.     

病毒感染对NLRP3炎症小体活化、组装和效应的影响

炎症小体是存在于胞浆的大分子多蛋白复合物,在感染或应激状态下被激活,并触发IL-1β和IL-18等促炎细胞因子的释放,诱导细胞焦亡,从而参与先天免疫防御。NLRP3识别病毒复制过程中产生的各种病原体相关分子模式（PAMP）和危险相关分子模式（DAMP）,启动NLRP3炎症小体依赖的抗病毒免疫反应。但是,有些病毒也进化出复杂的策略而靶向炎症小体,以逃避天然免疫监视。本综述讨论了病毒感染过程对NLRP3炎症小体的活化、组装和效应的影响。     

NLRP1炎性体

核苷酸结合寡聚化结构域样受体蛋白1(NLRP1)炎性体是NLRP1在识别胞内病原相关分子模式(PAMP)后与凋亡相关斑点样蛋白(ASC)以及半胱天冬氨酸酶(Caspase-1、Caspase-5)前体等分子结合形成的蛋白复合物,活化后促进IL-1β、IL-18、IL-33等炎症因子的成熟和释放,在先天性免疫中发挥重要作用。本文主要介绍了NLRP1炎性体的组成、激活机制、信号通路、负向调控及生物学功能,综述了NLRP1炎性体在炭疽、弓形虫病、泛发型白癜风、肠炎、牛皮癣等疾病中作用的研究进展。     

NLRP3炎性小体及其下游产物在TAO和ASO患者动脉中的表达及意义

目的:探讨NLRP3炎性小体及其下游产物在血栓闭塞性脉管炎(TAO)和动脉粥样硬化闭塞症(ASO)患者动脉中的表达及意义。方法:选择8例TAO患者截肢后的下肢动脉,13例ASO患者截肢后的下肢动脉,5例因窒息死亡的新生儿主动脉,将三组动脉分别进行HE染色及免疫组化分析,半定量的测量3组动脉中NLRP3、Caspase-1、IL-1β和IL-18的累积光密度值(IOD)并进行组间比较。结果:3组动脉组织的HE染色结果均符合其特征。TAO组和ASO组动脉组织中NLRP3、Caspase-1、IL-1β和IL-18的表达与对照组相比均显著升高,差异具有统计学意义(P0.05)。结论:NLRP3、Caspase-1、IL-1β和IL-18在TAO和ASO患者动脉组织中的表达明显升高,NLRP3炎性小体及其下游产物可能参与了TAO和ASO的发病过程。     

NLRP3炎症体与痛风的研究进展

痛风是由于机体血尿酸过饱和形成针状尿酸盐(Monosodium urate,MSU)沉积在关节腔导致的炎症。IL-1β是急性痛风性关节炎进程中重要的细胞因子,与炎症的产生以及炎症的级联放大反应有关,IL-1β的产生与细胞中炎症小体NLRP3复合体密切相关。研究者认为NLRP3炎症体是痛风性关节炎反应进程中的关键环节,痛风也被称为NLRP3炎症体相关疾病。本文综述了NLRP3炎症体与痛风的关系、相关机制,以及靶向NLRP3炎症体的小分子抑制剂,为今后寻找结构新颖、高效低毒的抗痛风新药的研究提供参考。     

食源性致病菌激活NLRP3炎症小体及食源性功能物质的抑制机理研究进展

食源性致病菌感染是引起食源性疾病的首要因素,严重影响人类健康。炎症小体通过识别受体感知入侵宿主的危险信号进而组装形成多聚蛋白复合物,从而诱导炎症反应,是先天免疫系统中识别食源性病原菌感染和清除病原体的重要防线。NLRP3炎症小体是位于胞内的炎症反应平台,可以感知多种病原微生物的侵袭,在先天性免疫反应中起着至关重要的作用。食源性致病菌感染常引起NLRP3炎症小体的异常激活,介导多种炎症性疾病的发生和发展,因此,许多抗炎研究中常常以NLRP3炎症小体作为靶点。本文总结了食源性致病菌及其代谢产物激活NLRP3炎症小体的分子机制,以及天然产物和膳食功能物质抑制NLRP3炎症小体激活的机理,为治疗炎症性疾病、开发缓解致病菌诱导的炎症反应的功能化合物提供新的思路。     

NLRP3炎性体与代谢性疾病的研究进展

代谢性疾病是由体内氨基酸、葡萄糖和脂质代谢紊乱引起的一类疾病,慢性炎症反应是其重要特征之一.Nod样受体蛋白3(Nod-like receptor protein 3,NLRP3)炎性体是位于细胞内的一种蛋白质复合体,主要功能为活化半胱氨酸天冬氨酸蛋白酶1(caspase-1)以间接调控白介素1β(IL-1β)、IL-18和IL-33等的成熟和分泌.NLRP3炎性体是炎性体相关研究的热点,多种内源性或外源性危险信号通过激活这一蛋白质复合体上调炎性因子的表达水平,从而促进多种代谢性疾病的发生发展.本文对NLRP3炎性体的结构、功能、调节以及在代谢性疾病中的作用做一综述,以期为代谢性疾病的防治提供新靶点.     

Bacterial infection reinforces host metabolic flux from arginine to spermine for NLRP3 inflammasome evasion

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The role of NLRP3-CASP1 in inflammasome-mediated neuroinflammation and autophagy dysfunction in manganese-induced,hippocampal-dependent impairment of learning and memory ability

Central nervous system (CNS) inflammation and autophagy dysfunction are known to be involved in the pathology of neurodegenerative diseases. Manganese (Mn), a neurotoxic metal, has the potential to induce microglia-mediated neuroinflammation as well as autophagy dysfunction. NLRP3 (NLR family, pyrin domain containing 3)- CASP1 (caspase 1) inflammasome-mediated neuroinflammation in microglia has specific relevance to neurological diseases. However, the mechanism driving these phenomena remains poorly understood. We demonstrate that Mn activates the NLRP3-CASP1 inflammasome pathway in the hippocampus of mice and BV2 cells by triggering autophagy-lysosomal dysfunction. The autophagy-lysosomal dysfunction is induced by lysosomal damage caused by excessive Mn accumulation, damaging the structure and normal function of these organelles. Additionally, we show that the release of lysosomal CTSB (cathepsin B) plays an important role in Mn-induced NLRP3-CASP1 inflammasome activation, and that the increased autophagosomes in the cytoplasm are not the main cause of NLRP3-CASP1 inflammasome activation. The accumulation of proinflammatory cytokines, such as IL1B (interleukin 1 β) and IL18 (interleukin 18), as well as the dysfunctional autophagy pathway may damage hippocampal neuronal cells, thus leading to hippocampal-dependent impairment in learning and memory, which is associated with the pathogenesis of Alzheimer disease (AD).     

小檗碱通过抑制经典的NLRP3炎症小体活化通路来下调LPS诱导的HUVEC炎症反应*

目的:探讨小檗碱(Berberine, Ber)对脂多糖(Lipopolysaccharide, LPS)诱导的人脐静脉血管内皮细胞(Human Umbilical VeinEndothelial Cells, HUVEC)炎症反应的抑制作用及相关机制。方法:MTT法检测不同浓度的Ber对HUVEC存活率的影响。以0.05μg/mL LPS刺激HUVEC建立炎症反应模型,并分别给予1.25、2.5、5μM Ber干预,Elisa检测Ber对炎症因子TNF-α、IL-1β分泌的影响,免疫印迹法检测Ber对NLRP3炎症小体信号通路中NLRP3、My D88、IL-1β、TLR4、ASC和Caspase-1蛋白表达的影响。结果:不同浓度的Ber对HUVEC增殖均具有抑制作用,且基本呈现浓度梯度,IC50值接近5μM;与LPS组相比,不同浓度Ber(1.25、2.5、5μM)均可以显著下调HUVEC中TNF-α、IL-1β炎症因子的分泌(P0.005及P0.01),并可以显著抑制细胞中NLRP3、My D88、IL-1β、TLR4、ASC和Caspase-1蛋白的表达(P0.05),其抑制作用基本呈剂量关系,以5μM Ber的抑制效果最佳。结论:Ber可以通过抑制经典的NLRP3炎症小体活化通路来下调LPS诱导的HUVEC炎症反应。     

Biological functions of NLRP3 inflammasome: A therapeutic target in inflammatory bowel disease

Cases of inflammatory bowel disease (IBD), a debilitating intestinal disorder with complex pathological mechanisms, have been increasing in recent years, straining the capacity of healthcare systems. Thus, novel therapeutic targets and innovative agents must be developed. Notably, the NLRP3 inflammasome is upregulated in patients with IBD and/or in animal experimental models. As an innate immune supramolecular assembly, the NLRP3 inflammasome is persistently activated during the pathogenesis of IBD by multiple stimuli. Moreover, this protein complex regulates pro-inflammatory cytokines. Thus, targeting this multiprotein oligomer may offer a feasible way to relieve IBD symptoms and improve clinical outcomes. The mechanisms by which the NLRP3 inflammasome is activated, its role in IBD pathogenesis, and the drugs administered to target this protein complex are reviewed herein. This review establishes that the use of inflammasome-targeting drugs are effective for IBD treatment. Moreover, this review suggests that the value and potential of naturally sourced or derived medicines for IBD treatment must be recognized and appreciated.     

人参皂苷Rg3通过调节自噬减轻脓毒症心肌损伤

摘要 目的：探讨人参皂苷Rg3（ginsenoside Rg3,Rg3）对脓毒症介导的心肌损伤的作用效果及机制。方法：本研究通过对小鼠进行盲肠结扎穿孔手术的方法构建脓毒症模型。32只BALB/c小鼠随机分为假手术组（Sham组）、脓毒症组（CLP组）、人参皂苷Rg3治疗组（Rg3+CLP组）以及自噬抑制剂干预组（3-MA+Rg3+CLP组）,每组8只。术后18 h分别留取各组小鼠血浆及心肌组织。通过ELISA方法检测白细胞介素-1β（IL-1β）、白细胞介素-18（IL-18）、乳酸脱氢酶（LDH）、肌酸激酶同工酶MB（CK-MB）及半胱氨酸蛋白酶-3（Caspase-3）表达水平。通过HE染色观察心肌组织形态结构的变化。应用Western-blot方法检测自噬及NLRP3炎性小体相关蛋白（NLRP3、ASC、Caspase-1）的表达。结果：与Sham组相比,CLP组小鼠心肌组织结构紊乱,炎性细胞浸润明显。另外,Caspase-3活性增加,NLRP3炎性小体相关蛋白（NLRP3、ASC、Caspase-1）表达升高,差异均有统计学意义（P＜0.05）。与CLP组相比,外源应用Rg3组小鼠心肌组织炎性细胞浸润减少,并且Caspase-3活性降低,NLRP3炎性小体相关蛋白表达下降,差异有统计学意义（P＜0.05）,而部分自噬相关蛋白表达升高。应用自噬抑制剂后,较单纯应用Rg3组,心肌组织损伤明显,而NLRP3炎性小体活性增加,差异有统计学意义（P＜0.05）。结论：脓毒症时NLRP3炎性小体激活,释放大量的细胞因子,进而导致心肌损伤。而Rg3治疗后,可以调节心肌细胞自噬,抑制NLRP3炎性小体激活,进而减轻细胞因子对心肌细胞的损伤。本研究表明Rg3可能通过调节心肌自噬,抑制NLRP3炎性小体的激活,进而减轻脓毒症时心脏的损伤。     

Activation of CXCR7 promotes endothelial repair and reduces the carotid atherosclerotic lesions through inhibition of pyroptosis signaling pathways

Endothelial injuries, including cell pyroptosis, are ongoing inflammatory processes with key roles in atherosclerosis development. Our previous report showed that the chemokine CXCL12 and its receptor CXCR7 are associated with the proliferation and angiogenesis of endothelial cells. Nevertheless, the mechanism underlying these effects on atherosclerotic lesions, especially on endothelial dysfunction, remains unknown. Here, we demonstrated that CXCR7 was upregulated in human carotid atherosclerotic plaques, apolipoprotein E knockout (ApoE^?/?) mice fed with a high‐fat diet (HFD), and oxidized lipopolysaccharide‐treated (ox‐LDL) human umbilical vein endothelial cells (HUVECs). Further, the activation of CXCR7 reversed ox‐LDL‐induced HUVEC dysfunction, such as migration, tube formation, and cell pyroptosis; all of these protective effects were alleviated by inhibition of CXCR7. The NOD‐like receptor family pyrin domain‐containing 3 (NLRP3) inflammasomes were also elevated in human carotid atherosclerotic plaques, ApoE^?/? mice fed with HFD, and ox‐LDL‐injured HUVECs by regulation of caspase‐1 and interleukin (IL)‐1β expression. The activation of CXCR7 by TC14012 led to a decrease in atherosclerotic lesions in ApoE^?/? mice fed with HFD. TC14012 also inhibited the expression of the NLRP3 inflammasome signaling pathway in vivo. In conclusion, our study suggests that CXCR7 plays an important role in regulating NLRP3 inflammasome‐modulated pyroptosis in HUVECs, providing a potential novel therapy for atherosclerosis.     

胆固醇结晶激活动脉粥样硬化斑块巨噬细胞NLRP3炎症体的途径

动脉粥样硬化既是胆固醇在血管壁聚集的疾病,也是发生在动脉壁的一种低强度慢性炎症形式。近年来有研究证实胆固醇结晶在动脉粥样硬化发生发展中具有重要作用。新的显微技术证实,胆固醇结晶在动脉粥样硬化斑块形成的早期即已出现,并与早期炎症有关。胆固醇结晶通过诱发局部炎症,促进大的脂质核心形成;刺破纤维帽,导致斑块破裂进而促进动脉粥样硬化斑块的进展。在影响斑块进程中,NLRP3炎症体的激活对此发挥了重要的作用。NLRP3炎症体是研究最多最明确的炎症体,其与非炎症性疾病的发生发展密切相关。以胆固醇结晶激活NLRP3炎症体的途径作为研究靶点,为动脉粥样硬化的诊断和治疗提供了新的思路和方法。该文就胆固醇结晶在动脉粥样硬化斑块中激活巨噬细胞NLRP3炎症体的两种途径做一综述。     

慢性PM2.5暴露对C57BL/6J小鼠肺组织炎症和NLRP3炎性小体活性的影响

目的 研究慢性PM2.5暴露对小鼠肺炎症和NLRP3炎性小体活性的影响,为防治PM2.5所致肺损伤提供新靶点。方法 雄性C57BL/6J小鼠通过不同剂量气管滴注法进行PM2.5染毒,剂量为2,10mg/(kg·bw),对照组小鼠滴注生理盐水。小鼠连续滴注20次,每3d染毒1次后,取血和肺组织。三组小鼠进行血细胞计数;用免疫荧光染色法检测肺组织巨噬细胞水平;用试剂盒测定肺组织中白细胞介素(interleukin,IL)-1β,IL-18水平及caspase-1活性;用实时定量PCR法检测肺组织NLRP3炎性小体相关mRNA表达水平。结果 两个剂量PM2.5染毒均能明显降低单核细胞百分比(P<0.01),增加中性粒白细胞百分比(P<0.01);导致肺炎症发生;增加肺组织caspase-1活性(P<0.01)及NLRP3和ASC的mRNA表达(P<0.01)。与对照组相比,两个剂量组小鼠肺组织IL-1β和IL-18水平均显著增高(P<0.01)。结论 慢性PM2.5暴露可能通过激活肺组织NLRP3炎性小体导致肺炎症发生。     

Cancer and Covid-19: Collectively catastrophic

The Covid-19 pandemic has spread rapidly across the globe, resulting in more than 3 million deaths worldwide. The symptoms of Covid-19 are usually mild and non-specific, however in some cases patients may develop acute respiratory distress syndrome (ARDS) and systemic inflammation. Individuals with inflammatory or immunocompromising illnesses, such as cancer, are more susceptible to develop ARDS and have higher rates of mortality. This is mediated through an initial hyperstimulated immune response which results in elevated levels of pro-inflammatory cytokines and a subsequent cytokine storm. This potentiates positive feedback loops which are unable to be balanced by anti-inflammatory mediators. Therefore, elevated levels of IL-1β, as a result of NLRP3 inflammasome activation, as well as IL-6 and TNF-α amongst many others, contribute to the progression of various cancer types. Furthermore, Covid-19 progression is associated with the depletion of CD8⁺ and CD4⁺ T cells, B cell and natural killer cell numbers. Collectively, a Covid-19-dependent pro-inflammatory profile and immune suppression promotes the optimal microenvironment for tumourigenesis, initiation and immune evasion of malignant cells, tumour progression and metastasis as well as cancer recurrence. There are, however, therapeutic windows of opportunity that may combat both Covid-19 and cancer to improve patient outcomes.     

NLRP3 inflammasome inhibition attenuates silica-induced epithelial to mesenchymal transition (EMT) in human bronchial epithelial cells

Silicosis is an incurable and progressive lung disease characterized by chronic inflammation and fibroblasts accumulation. Studies have indicated a vital role for epithelial-mesenchymal transition (EMT) in fibroblasts accumulation. NLRP3 inflammasome is a critical mediator of inflammation in response to a wide range of stimuli (including silica particles), and plays an important role in many respiratory diseases. However, whether NLRP3 inflammasome regulates silica-induced EMT remains unknown. Our results showed that silica induced EMT in human bronchial epithelial cells (16HBE cells) in a dose- and time-dependent manner. Meanwhile, silica persistently activated NLRP3 inflammasome as indicated by continuously elevated extracellular levels of interleukin-1β (IL-1β) and IL-18. NLRP3 inflammasome inhibition by short hairpin RNA (shRNA)-mediated knockdown of NLRP3, selective inhibitor MCC950, and caspase-1 inhibitor Z-YVAD-FMK attenuated silica-induced EMT. Western blot analysis indicated that TAK1-MAPK-Snail/NF-κB pathway involved NLRP3 inflammasome-mediated EMT. Moreover, pirfenidone, a commercially and clinically available drug approved for treating idiopathic pulmonary fibrosis (IPF), effectively suppressed silica-induced EMT of 16HBE cells in line with NLRP3 inflammasome inhibition. Collectively, our results indicate that NLRP3 inflammasome is a promising target for blocking or retarding EMT-mediated fibrosis in pulmonary silicosis. On basis of this mechanism, pirfenidone might be a potential drug for the treatment of silicosis.     

NLRP6在感染性和非感染性疾病中的作用

核苷酸结合寡聚化结构域样受体含pyrin结构域蛋白6(NLRP6)属于核苷酸结合寡聚化结构域样受体(NLRs)家族蛋白.NLRP6可以作为受体蛋白参与炎症小体的组装,引起白细胞介素IL-1β和IL-18的成熟与分泌.NLRP6在病原体感染诱导宿主天然免疫应答中发挥重要作用.此外,NLRP6在维持肠道上皮完整、调控代谢性...