Protective effects of IRG1/itaconate on acute colitis through the inhibition of gasdermins-mediated pyroptosis and inflammation response

Inflammatory bowel disease(IBD)is a chronic relapsing gastrointestinal disorder,while the treatment effect is not satisfactory.Immune responsive gene 1(IRG1)is a highly ex-pressed gene in macrophage in response to inflammatory response and catalyzes the production of itaconate.Studies have reported that IRG1/itaconate has a significant antioxidant effect.This study aimed to investigate the effect and mechanism of IRG1/itaconate on dextran sulfate so-dium(DSS)-induced colitis in vivo and in vitro.In vivo experiments,we found IRG1/itaconate ex-erted protective effects against acute colitis by increasing mice weight,the length of colon,reducing disease activity index and colonic inflammation.Meanwhile,IRG1 deletion aggravated the macrophages/CD4+/CD8+T-cell accumulation,and increased the release of interleukin(IL)-1b,tumor necrosis factor-a(TNF-a),IL-6,the activation of nuclear factor-kB(NF-kB)/mitogen-activated protein kinase(MAPK)signaling pathway,and gasdermin D(GSDMD)mediated pyrop-tosis.Four-octyl itaconate(4-OI),a derivative of itaconate,attenuated these changes,therefore relieved DSS-induced colitis.In vitro experiment,we found 4-OI inhibited the reactive oxygen species production,thereby inhibiting the activation of MAPK/NF-kB signaling pathway in RAW264.7 and murine bone-marrow-derived macrophages.Simultaneously,we found 4-OI inhib-ited caspase1/GSDMD-mediated pyroptosis to reduce the release of cytokines.Finally,we found anti-TNF-a agent reduced the severity of DSS-induced colitis and inhibited gasdermin E(GSDME)-mediated pyroptosis in vivo.Meanwhile,our study revealed that 4-OI inhibited caspase3/GSDME-mediated pyroptosis induced by TNF-a in vitro.Taken together,IRG1/itaconate exerted a pro-tective role in DSS-induced colitis by inhibiting inflammatory response and GSDMD/GSDME-medi-ated pyroptosis,which could be a promising candidate for IBD therapy.

脊髓损伤后细胞焦亡调控机制及治疗策略

背景:调节细胞死亡和神经炎症是治疗脊髓损伤的两个重要途径,细胞焦亡是一种与神经炎症密切相关的程序性死亡模式,针对性靶向抑制脊髓损伤后焦亡,是一项有前景的治疗策略。目的:归纳细胞焦亡在脊髓损伤中的分子机制、正负向调节因子及治疗策略的研究进展。方法:以“spinal cord injury,pyroptosis,nucleotide-binding oligomerization domain-like receptor protein 3(NLRP3),Caspase,Gasdermin D(GSDMD),IL-1β,IL-18”为检索词,在PubMed和Web of Science数据库进行检索,最终纳入93篇英文文献。结果与结论:①作为新发现的程序性死亡方式,细胞焦亡已被证实在脊髓损伤后继发性损伤阶段起重要作用。②在脊髓损伤后细胞焦亡的调节因子中,CD73、NRF2、GDF-11、多巴胺、FANCC和miR-423-5P可抑制细胞焦亡,TLR4和Aopps可促进细胞焦亡。③在治疗策略方面,中药活性成分丹皮酚、雷公藤红素、桦木酸、胡椒碱、山奈酚、喜树碱,各种细胞来源的外泌体,药物二甲双胍、拓扑替康、锂、锌和一氧化碳释放分子3能有效抑制焦亡,减轻脊髓继发性损伤,但这些药物的毒副反应和具体剂量有待深入研究。④细胞焦亡加重脊髓损伤的具体分子机制仍知之甚少,非经典途径及其他炎性小体的作用值得进一步探索。⑤目前脊髓损伤后焦亡的研究仅停留在动物实验阶段,尚无相关临床研究,且无批准的靶向治疗药物。⑥细胞焦亡在脊髓损伤后的应用具有巨大潜能,未来需继续研究其具体调控机制,为脊髓损伤的治疗提供新的作用靶点。

Silent information regulator sirtuin 1 ameliorates acute liver failure via the p53/glutathione peroxidase 4/gasdermin D axis

BACKGROUND Acute liver failure(ALF)has a high mortality with widespread hepatocyte death involving ferroptosis and pyroptosis.The silent information regulator sirtuin 1(SIRT1)-mediated deacetylation affects multiple biological processes,including cellular senescence,apoptosis,sugar and lipid metabolism,oxidative stress,and inflammation.AIM To investigate the association between ferroptosis and pyroptosis and the upstream regulatory mechanisms.METHODS This study included 30 patients with ALF and 30 healthy individuals who underwent serum alanine aminotransferase(ALT)and aspartate aminotransferase(AST)testing.C57BL/6 mice were also intraperitoneally pretreated with SIRT1,p53,or glutathione peroxidase 4(GPX4)inducers and inhibitors and injected with lipopolysaccharide(LPS)/D-galactosamine(D-GalN)to induce ALF.Gasdermin D(GSDMD)^(-/-)mice were used as an experimental group.Histological changes in liver tissue were monitored by hematoxylin and eosin staining.ALT,AST,glutathione,reactive oxygen species,and iron levels were measured using commercial kits.Ferroptosis-and pyroptosis-related protein and mRNA expression was detected by western blot and quantitative real-time polymerase chain reaction.SIRT1,p53,and GSDMD were assessed by immunofluorescence analysis.RESULTS Serum AST and ALT levels were elevated in patients with ALF.SIRT1,solute carrier family 7a member 11(SLC7A11),and GPX4 protein expression was decreased and acetylated p5,p53,GSDMD,and acyl-CoA synthetase long-chain family member 4(ACSL4)protein levels were elevated in human ALF liver tissue.In the p53 and ferroptosis inhibitor-treated and GSDMD^(-/-)groups,serum interleukin(IL)-1β,tumour necrosis factor alpha,IL-6,IL-2 and C-C motif ligand 2 levels were decreased and hepatic impairment was mitigated.In mice with GSDMD knockout,p53 was reduced,GPX4 was increased,and ferroptotic events(depletion of SLC7A11,elevation of ACSL4,and iron accumulation)were detected.In vitro,knockdown of p53 and overexpression of GPX4 reduced AST and ALT levels,the cytostatic rate,and GSDMD expression,restoring SLC7A11 depletion.Moreover,SIRT1 agonist and overexpression of SIRT1 alleviated acute liver injury and decreased iron deposition compared with results in the model group,accompanied by reduced p53,GSDMD,and ACSL4,and increased SLC7A11 and GPX4.Inactivation of SIRT1 exacerbated ferroptotic and pyroptotic cell death and aggravated liver injury in LPS/D-GalNinduced in vitro and in vivo models.CONCLUSION SIRT1 activation attenuates LPS/D-GalN-induced ferroptosis and pyroptosis by inhibiting the p53/GPX4/GSDMD signaling pathway in ALF.

细胞焦亡在肿瘤免疫中的研究进展

细胞焦亡作为宿主防御的主要机制,是连接先天免疫和适应性免疫的关键。伴随胞膜破裂,焦亡细胞释放出大量的炎症介质,招募炎症细胞,激活炎症反应。肿瘤免疫治疗是利用宿主的天然防卫机制,给予某些免疫调节剂、抗体或者经过刺激调整后的免疫细胞,以取得更强的抗肿瘤效应。最近的研究表明:细胞焦亡对肿瘤免疫治疗有正向调控作用,包括免疫检查点抑制剂和嵌合抗原受体T细胞免疫治疗等。本文就焦亡机制及其与肿瘤免疫治疗的相关性,结合已发表实验研究,阐明细胞焦亡在肿瘤免疫中的作用机制,以期为恶性肿瘤基础和临床研究提供新思路。

细胞焦亡的作用机制及其在脓毒症中的研究进展

脓毒症是可导致机体严重器官功能障碍、危及生命的炎性综合反应,一般是由病原微生物侵入机体引发,近年来发生率和病死率居高不下,是重症监护病房患者死亡的重要原因。细胞焦亡是新发现的一种伴随炎症因子释放的细胞程序性死亡,可一定程度上抵御微生物的感染,但过度激活会诱导和加重脓毒症。目前有研究证明,细胞焦亡的许多相关分子都参与了脓毒症的发病进程,并在其中发挥重要作用。对脓毒症中细胞焦亡的研究不仅可深入阐明细胞焦亡的病理作用和机制,也有助于对脓毒症的发生发展和转归预判,尤其为发现治疗脓毒症的靶点拓展新思路。

GSDMD介导细胞焦亡缓解高尿酸血症小鼠肾损伤的作用机制

目的:探讨gasdermin D蛋白(GSDMD)在高尿酸血症(HUA)后肾损伤中的作用及其可能机制。方法:选用C57BL/6J的野生型小鼠和GSDMD敲除小鼠作为实验动物,将其分为4组,野生型小鼠正常饮食组(WT-Norm-diet组),野生型小鼠高尿酸造模组(WT-HUA组),GSDMD敲除小鼠正常饮食组(KO-Norm-diet组)和GSDMD敲除小鼠高尿酸造模组(KO-HUA组)。HUA动物造模选用氧嗪酸钾[250 mg/(kg·d)]和腺嘌呤[50 mg/(kg·d)]对小鼠灌胃28 d;血生化检测肌酐和尿酸变化;HE染色观察肾脏病理学变化;Western blot检测肾皮质GSDMD、GSDMD-N的蛋白表达;RT-PCR检测KIM-1和NAGL的表达量。结果:与WT-Norm-diet组比较,WT-HUA组小鼠血清中尿酸升高(P<0.01);肾皮质中GSDMD、GSDMD-N的蛋白表达水平升高(P<0.05);KIM-1 mRNA的表达水平升高(P<0.01)。与WT-HUA组比较,KO-HUA组小鼠血清尿酸、肌酐水平、NAGL mRNA表达降低(P<0.05)。HE染色结果显示,KO-HUA组小鼠高尿酸导致的肾小管扩展以及炎性细胞浸润明显改善。结论:GSDMD敲除可有效缓解高尿酸引起的肾脏损伤。

Understanding the molecular crossroads in acute liver failure:A pathway to new therapies

In this editorial we comment on the article published in a recent issue of the World Journal of Gastroenterology.Acute liver failure(ALF)is a critical condition characterized by rapid hepatocellular injury and organ dysfunction,and it often necessitates liver transplant to ensure patient survival.Recent research has eluci-dated the involvement of distinct cell death pathways,namely ferroptosis and pyroptosis,in the pathogenesis of ALF.Ferroptosis is driven by iron-dependent lipid peroxidation,whereas pyroptosis is an inflammatory form of cell death;both pathways contribute to hepatocyte death and exacerbate tissue damage.This comprehensive review explores the interplay between ferroptosis and pyroptosis in ALF,highlighting the role of key regulators such as silent information regulator sirtuin 1.Insights from clinical and preclinical studies provide valuable perspectives on the dysregulation of cell death pathways in ALF and the therapeutic potential of targeting these pathways.Collaboration across multiple disciplines is essential for translating the experimental insights into effective treatments for this life-threatening condition.

Overview of ferroptosis and pyroptosis in acute liver failure

In this editorial,we comment on the article by Zhou et al published in a recent issue.We specifically focus on the crucial roles of ferroptosis and pyroptosis in acute liver failure(ALF),a disease with high mortality rates.Ferroptosis is the result of increased intracellular reactive oxygen species due to iron accumulation,glutathione(GSH)depletion,and decreased GSH peroxidase 4 activity,while pyroptosis is a procedural cell death mediated by gasdermin D which initiates a sustained inflammatory process.In this review,we describe the characteristics of ferroptosis and pyroptosis,and discuss the involvement of the two cell death modes in the onset and development of ALF.Furthermore,we summarize several interfering methods from the perspective of ferroptosis and pyroptosis for the alleviation of ALF.These observations might provide new targets and a theoretical basis for the treatment of ALF,which are also crucial for improving the prognosis of patients with ALF.

Sirtuin 1 in regulating the p53/glutathione peroxidase 4/gasdermin D axis in acute liver failure

In this editorial,we comment on the article by Zhou et al.The study reveals the connection between ferroptosis and pyroptosis and the effect of silent information regulator sirtuin 1(SIRT1)activation in acute liver failure(ALF).ALF is characterized by a sudden and severe liver injury resulting in significant hepatocyte damage,often posing a high risk of mortality.The predominant form of hepatic cell death in ALF involves apoptosis,ferroptosis,autophagy,pyroptosis,and necroptosis.Glutathione peroxidase 4(GPX4)inhibition sensitizes the cell to ferroptosis and triggers cell death,while Gasdermin D(GSDMD)is a mediator of pyroptosis.The study showed that ferroptosis and pyroptosis in ALF are regulated by blocking the p53/GPX4/GSDMD pathway,bridging the gap between the two processes.The inhibition of p53 elevates the levels of GPX4,reducing the levels of inflammatory and liver injury markers,ferroptotic events,and GSDMDN protein levels.Reduced p53 expression and increased GPX4 on deletion of GSDMD indicated ferroptosis and pyroptosis interaction.SIRT1 is a NAD-dependent deacetylase,and its activation attenuates liver injury and inflammation,accompanied by reduced ferroptosis and pyroptosis-related proteins in ALF.SIRT1 activation also inhibits the p53/GPX4/GSDMD axis by inducing p53 acetylation,attenuating LPS/D-GalN-induced ALF.

Targeting both ferroptosis and pyroptosis may represent potential therapies for acute liver failure

In this editorial,we comment on the article published in the recent issue of the World Journal of Gastroenterology.Acute liver failure(ALF)is a fatal disease that causes uncontrolled massive hepatocyte death and rapid loss of liver function.Ferroptosis and pyroptosis,cell death forms that can be initiated or blocked concurrently,can play significant roles in developing inflammation and various malignancies.However,their roles in ALF remain unclear.The article discovered the positive feedback between ferroptosis and pyroptosis in the progression of ALF,and revealed that the silent information regulator sirtuin 1(SIRT1)inhibits both pathways through p53,dramatically reducing inflammation and protecting hepatocytes.This suggests the potential use of SIRT1 and its downstream molecules as therapeutics for ALF.Thus,we will discuss the role of ferroptosis and pyroptosis in ALF and the crosstalk between these cell death mechanisms.Additionally,we address potential treatments that could alleviate ALF by simultaneously inhibiting both cell death pathways,as well as examples of SIRT1 activators being used as disease treatment strategies,providing new insights into the therapy of ALF.

GSDMB调控肠上皮细胞命运的分子机制初探

目的初步探讨Gasdermin B(GSDMB)调控肠上皮细胞命运的分子机制。方法过表达人GSDMB质粒到两种人肠上皮细胞系(NCM460和HT-29细胞)和人结肠类器官中,采用免疫印迹法(Western blotting)检测电转效率,并利用细胞计数试剂盒(CCK8),流式细胞术检测细胞凋亡和细胞周期以分析GSDMB过表达对细胞功能的影响。转录组测序分析GSDMB的下游效应分子。组间数据比较采用t检验。结果成功重构两种肠上皮细胞系GSDMB蛋白过表达,过表达GSDMB蛋白的人肠上皮细胞吸光度值(A)[NCM460细胞:(1.17±0.01);HT-29细胞:(0.96±0.06)]明显低于空白对照组[NCM460细胞:(1.67±0.12);HT-29细胞:(1.24±0.07)],差异有统计学意义(t=7.24、5.46,P<0.05);GSDMB过表达组细胞凋亡数目[NCM460细胞:(12.03±1.55);HT-29细胞:(29.30±4.48)]显著多于空白对照组[NCM460细胞:(4.96±1.74);HT-29细胞:(6.95±3.42)],差异有统计学意义(t=5.26、6.97,P<0.05);细胞周期分析显示,GSDMB过表达组细胞G0/G1期比例[NCM460细胞:(47.98±5.28)%;HT-29细胞:(38.04±3.45)%]明显低于空白对照组[NCM460细胞:(59.54±3.90)%;HT-29细胞:(63.81±1.76)%],差异有统计学意义(t=3.05、11.53,P<0.05)。转录组测序结果发现,双特异性磷酸酶4和6(DUSP4和DUSP6)基因在肠上皮细胞表达GSDMB蛋白后显著上调,荧光定量PCR结果证实肠上皮细胞转染GSDMB后DUSP4(2.45±0.15)和DUSP6(4.34±0.22)相对表达水平显著高于对照组(1.06±0.05和1.01±0.02),差异有统计学意义(t=15.08、26.52,P<0.05)。使用DUSP抑制剂BCI处理重构GSDMB表达的NCM460细胞,发现BCI处理组p-ERK表达水平相对于对照组显著升高[(1.14±0.17)vs.(0.58±0.12)],差异有统计学意义(t=5.42,P=0.002),且BCI处理组细胞A值(1.84±0.07)和G0/G1期比例(59.83±2.17)%高于未处理组[(1.52±0.10)和(52.10±2.23)%],BCI处理组细胞凋亡数目(7.60±0.56)明显少于未处理组(12.57±1.00),差异均有统计学意义(t=4.71、4.31、7.52,P<0.05)。过表达GSDMB后的人结肠类器官TUNEL染色提示凋亡的细胞明显增多,DUSP6蛋白相对表达水平(0.85±0.09)显著高于对照组(0.21±0.04),同时伴随p-ERK水平的下降[(0.83±0.18)vs.(0.19±0.06)],差异有统计学意义(t=11.95,P<0.001;t=6.56,P<0.001)。结论GSDMB可能通过调节DUSP6介导的ERK信号来抑制细胞增殖,诱导细胞周期阻滞,促进细胞凋亡,从而影响肠上皮细胞命运。

口腔癌组织中GSDME、SAA1的表达情况及其与患者临床病理特征及预后的关系

目的分析口腔癌组织中Gasdermin E(GSDME)、血清淀粉样蛋白A1(SAA1)的表达情况,并探讨两者与口腔癌患者临床病理特征及预后的关系。方法选取102例口腔癌患者,采用免疫组织化学法检测癌组织和癌旁组织中GSDME、SAA1的表达情况。分析不同临床病理特征患者口腔癌组织中GSDME、SAA1的表达情况。采用Kaplan⁃Meier法绘制生存曲线,分析癌组织中GSDME、SAA1的表达情况与患者预后的关系。采用多因素COX回归模型分析口腔癌患者预后的影响因素。结果口腔癌组织中GSDME表达阳性率低于癌旁组织,SAA1表达阳性率高于癌旁组织(P<0.05)。相比于高中分化程度、无颈淋巴结转移、TNM分期Ⅰ~Ⅱ期患者,低分化程度、有颈淋巴结转移、TNM分期Ⅲ期患者癌组织的GSDME表达阳性率较低,SAA1表达阳性率较高(P<0.05)。GSDME表达阴性患者的3年无进展生存率低于GSDME表达阳性患者(P<0.05);SAA1表达阳性患者的3年无进展生存率低于SAA1蛋白阴性患者(P<0.05)。分化程度、颈淋巴结转移、TNM分期、癌组织GSDME和SAA1表达情况是口腔癌患者预后的独立影响因素(P<0.05)。结论口腔癌组织中GSDME表达降低、SAA1表达升高,两者与患者的TNM分期、肿瘤细胞分化程度、颈淋巴结转移及预后密切相关。

Noncanonical pyroptosis pathway: a promising target of traditional Chinese medicine in the treatment of sepsis-related injury

Sepsis is a life-threatening disease of organ failure caused by dysregulated host responses to infection and other infectious factors.Multi-organ injury is the leading cause of high mortality and septic shock during sepsis.Recent studies suggest that noncanonical pyroptosis,characterized mainly by the direct activation of caspase-11-gasdermin D-mediated pyroptosis by cytoplastic lipopolysaccharide,is closely related to sepsis-related organ injury.Here,this review summarizes recent advances in the regulatory mechanisms and targeted natural products from traditional Chinese medicine of the noncanonical pyroptosis pathway in sepsis-related injury.

细胞焦亡在急性肾损伤中的研究进展

急性肾损伤(AKI)的主要病理特征是肾脏毛细血管内皮损伤引起的血管功能障碍、强烈的炎症反应和肾小管上皮细胞(TEC)损伤。细胞焦亡是由内源性细胞损伤〔损伤相关分子模式(DAMPs)〕或外源性细菌、病毒〔病原体相关分子模式(PAMPs)〕激活炎症小体相继引发下游信号活跃度增加的级联放大反应,是可导致细胞膜破坏且内容物大量释放的一种区别于凋亡的细胞死亡方式。近年来焦亡与AKI的关系也不断被报道且广受关注。现重点对细胞焦亡的分子机制及细胞焦亡与AKI关系的相关研究成果进行综述,以期为今后临床医生防治AKI提供帮助。

甘草附子汤加减方通过抑制GSDMD介导的焦亡治疗CIA大鼠的作用机制研究

目的:探讨甘草附子汤加减方(GCFZD)抑制gasdermin D (GSDMD)介导细胞焦亡途径对胶原诱导性关节炎(CIA)大鼠的治疗效果。方法:SD大鼠尾跟部注射由牛Ⅱ型胶原与弗氏佐剂混合形成的乳化剂,构建CIA大鼠模型并对其关节炎指数进行评估,将成功诱发关节炎的30只雄性SD大鼠随机分为模型组、甘草附子汤低(4 g/kg)、中(8 g/kg)和高(16 g/kg)剂量组及甲氨蝶呤(1 mg/kg)组,每组6只,连续给药30 d。测定大鼠的体重、关节炎指数和足爪肿胀指数;X线影像学观察骨质破坏和软组织厚度改变;HE染色观察脾脏和关节组织病理学改变;番红O-固绿染色观察关节软骨改变;TUNEL染色观察关节内细胞焦亡发生情况;Western blot测定TLR4、caspase-1、NLRP3和GSDMD蛋白表达;real-time PCR和ELISA测定IL-1β、IL-6和IL-10细胞因子表达。结果:与模型组相比,GCFZD治疗显著改善CIA大鼠软组织肿胀和骨质破坏,降低脾脏和胸腺指数;HE染色结果显示,GCFZD治疗减轻CIA大鼠脾脏和踝关节组织病理学改变;番红O-固绿染色结果显示,GCFZD治疗减少软骨组织破坏,修复软骨结构;TUNEL染色结果显示,GCFZD显著抑制关节组织内的细胞焦亡;Western blot结果表明,GCFZD降低CIA大鼠脾脏中TLR4、cleaved caspase-1、NLRP3和GSDMD-N的蛋白表达;real-time PCR和ELISA结果显示,GCFZD减少CIA大鼠IL-1β和IL-6的mRNA和蛋白水平的表达,上调IL-10的mRNA和蛋白水平的表达。结论:GCFZD能够抑制GSDMD介导的细胞焦亡,减少IL-1β和IL-6分泌,促进IL-10分泌,有效减轻CIA大鼠的类风湿关节炎症状。

细胞焦亡在肿瘤发生、发展与治疗中的作用

细胞焦亡(pyroptosis)又称细胞炎性坏死,是Gasdermin蛋白家族介导的一种程序性细胞死亡,表现为细胞不断肿胀直至细胞膜破裂,导致细胞内容物释放,进而激活强烈的炎症反应。近年来,细胞焦亡在肿瘤发病机制中的作用变得越来越突出,焦亡信号通路分子及细胞焦亡过程中释放的多种炎症介质与肿瘤的发生、发展及对肿瘤化疗和免疫治疗的反应密切相关。由于肿瘤的异质性,细胞焦亡在不同肿瘤中的作用并不相同,因此有必要研究细胞焦亡在不同肿瘤中的具体作用机制。从药理学角度,寻求促进生成炎症小体或激活焦亡通路的分子底物,为肿瘤药物的研发和治疗提供更多思路。细胞焦亡在一定程度上也解答了肿瘤化疗和免疫治疗副作用产生的原因。细胞焦亡在肿瘤治疗过程中是“双刃剑”,如何调节药物在肿瘤组织、正常组织和免疫微环境中诱导细胞焦亡的方式和程度,对于提高肿瘤的化疗和免疫治疗效果,降低毒副作用具有重要的意义。本文就细胞焦亡的类型及分子机制,细胞焦亡在肿瘤的发生发展及其在肿瘤化疗、放射治疗、中药治疗和免疫治疗过程中发挥的作用进行综述,以期为临床肿瘤治疗和预后分析提供新靶点。

清肺通络方通过胱天蛋白酶-1/Gasdermin D蛋白细胞焦亡途径对支原体肺炎小鼠的干预机制

目的:探讨清肺通络方通过胱天蛋白酶-1(Caspase-1)/Gasdermin D(GSDMD)蛋白细胞焦亡途径对支原体肺炎小鼠干预机制。方法:将30只BALB/c小鼠随机分为空白对照组、模型组、清肺通络方组,每组10只。采用肺炎支原体菌株滴鼻法建立支原体肺炎小鼠模型。造模同时予灌胃治疗,连续治疗3 d,实验第4天处死各组小鼠。PCR检测小鼠肺组织MP-DNA含量,HE染色观察小鼠肺组织病理改变,Western blot检测胱天蛋白酶-1前体(pro-Caspase-1)、Caspase-1、GSDMD、Gasdermin D氮端活性结构域多肽(GSDMD-N)表达,ELISA检测肺泡灌洗液中白介素-1β(IL-1β)、白介素-18(IL-18)含量,生化法检测肺组织细胞乳酸脱氢酶(LDH)和Na+-K+-ATP酶活性。结果:镜下观察模型组小鼠肺间质出现炎性细胞浸润、渗出明显。与空白对照组比较,模型组小鼠pro-Caspase-1、Caspase-1、GSDMD、GSDMD-N表达及IL-1β、IL-18含量均升高,LDH活性上升,Na+-K+-ATP酶活性下降(均P<0.05);与模型组比较,清肺通络方组小鼠肺间质炎症细胞浸润明显减轻,肺组织中Caspase-1、GSDMD、GSDMD-N表达及IL-1β、IL-18含量均降低(均P<0.05),LDH活性下降,Na+-K+-ATP酶活性上升(均P<0.05);两组pro-Caspase-1表达比较差异无统计学意义(P>0.05)。结论:清肺通络方通过抑制Caspase-1/GSDMD通路,缓解细胞焦亡,减轻小鼠肺组织炎症反应。

细胞焦亡参与早期子鼠坏死性小肠结肠炎的发病

目的通过建立坏死性小肠结肠炎的小鼠模型,检测新生子鼠发生NEC早期时血清中细胞焦亡的关键蛋白分子,从而初步判断细胞焦亡是否参与早期新生儿坏死性小肠结肠炎的发病。方法将新出生的子鼠随机分为实验组和对照组,实验组的子鼠诱导为NEC的动物模型,抽取2组子鼠血液,用Elisa试剂盒检测所有子鼠血清中IL-18、Gasdermin D、Caspase-1的浓度,运用秩和检验统计学方法,比较2组血清中目标蛋白的浓度,检验水准α=0.05。结果2组子鼠血清中Gasdermin D、Caspase-1的浓度差异有统计学意义,P值分别为0.017、<0.001,可认为实验组子鼠血清中Gasdermin D、Caspase-1的浓度高于对照组,2组血清中IL-18的浓度无明显差异,P=0.755。结论由Gasdermin D介导的细胞焦亡可能参与早期NEC的发病。

抑制肺泡上皮细胞焦亡对支气管肺发育不良新生大鼠肺泡化阻滞的改善作用

目的·研究gasderminD(GSDMD)抑制剂necrosulfonamide(NSA)通过抑制肺上皮细胞焦亡对脂多糖(lipopolysaccharide,LPS)诱导的新生大鼠支气管肺发育不良(bronchopulmonary dysplasia,BPD)肺泡化阻滞的影响。方法·将孕SD大鼠随机分为对照组、BPD组、BPD+NSA组和NSA组,羊膜腔注射LPS建立新生鼠BPD模型。取各组出生后第1、3、7日新生鼠肺组织,通过苏木精-伊红(H-E)染色观察肺泡化情况;利用免疫荧光法检测各组新生鼠肺部GSDMD-N端蛋白表达情况;荧光定量PCR法检测新生鼠肺组织中炎症因子白介素-1β(interleukin-1β,IL-1β)mRNA水平。体外培养小鼠肺泡上皮细胞系MLE-12,给予LPS以及腺苷三磷酸(adenosine triphosphate,ATP)刺激和NSA干预,CCK-8法检测MLE-12细胞活力,Hoechst 33342和碘化丙啶(propidium iodide,PI)染色法检测细胞焦亡水平,免疫荧光法检测MLE-12细胞表面活性剂蛋白C(surfactant protein C,SFTPC)和GSDMD-N端蛋白的表达情况。结果·体内实验结果显示:羊膜腔内注射LPS可导致肺发育受阻,模拟BPD的病理改变;羊膜腔内注射LPS建立的BPD模型中肺泡上皮细胞GSDMD-N端表达升高;NSA干预明显改善了BPD新生鼠的肺发育阻滞并抑制了IL-1β的mRNA表达(均P<0.05)。体外实验结果显示:LPS/ATP刺激下肺泡上皮细胞MLE-12活力下降,发生焦亡;NSA干预提高了肺泡上皮细胞活力并且抑制了焦亡(均P<0.05);NSA上调了LPS/ATP刺激下肺泡上皮细胞SFTPC的表达,抑制了LPS/ATP刺激下肺泡上皮细胞GSDMD-N端表达的上调(均P<0.05)。结论·抑制肺泡上皮细胞焦亡可改善LPS诱导的BPD新生鼠肺组织病理学改变。

GSDM家族蛋白在细胞焦亡中的作用研究进展

细胞焦亡作为炎性反应性的调控性细胞死亡,在生物体抵御外来病原体及各种临床疾病中发挥着重要作用,近年来焦亡通过Caspase激活的具体机制研究取得了突破性的进展,gasdermin D蛋白(GSDMD)作为Caspase底物被切割并发挥针对细胞膜的穿孔作用,诱导细胞焦亡,其他GSDMs家族蛋白在焦亡中的作用也逐渐被阐明。细胞焦亡已被认为是GSDM家族蛋白介导的程序性死亡过程,其在肿瘤及其他临床疾病中的机制研究显得越来越重要。文章就GSDM家族蛋白在细胞焦亡中的作用研究进展作一综述。