摘要
目的:研究诺达基因对小鼠克罗恩病(CD)样结肠炎的治疗机制:研究诺达凯宁对小鼠克罗恩病(CD)样结肠炎的治疗机制:方法:利用脂多糖(LPS)和ATP诱导的热蛋白沉积的结肠类器官模型,通过检测关键的热蛋白沉积调节因子以及评估渗透性和促炎因子的变化,研究诺达凯宁对热蛋白沉积、肠屏障功能和炎症反应的影响。在2,4,6-三硝基苯磺酸(TNBS)诱导的CD样结肠炎小鼠模型中,通过测量体重、DAI评分、结肠组织病理学、炎症评分、肠屏障功能和肠上皮细胞裂解的变化,评估了点头素的治疗效果。通过网络药理学分析以及体内和体外实验,探讨了点头草素保护肠上皮细胞不发生热缩的机制:结果:在LPS和ATP诱导的结肠器官组织中,诺达凯宁能显著抑制NLRP3、GSDMD-N、裂解的caspase-1和caspase-11的表达,改善肠道FITC-葡聚糖(FD4,4000)的通透性,降低IL-1β和IL-18的水平。在 TNBS 诱导的小鼠结肠炎模型中,诺达凯宁治疗可显著减轻体重下降,降低 DAI 评分、炎症细胞浸润和炎症评分,降低血清 FD4 和 I-FABP 水平以及肠系膜淋巴结、脾脏和肝脏的细菌转位。接受点头素治疗的小鼠肠粘膜中的NLRP3、GSDMD-N、裂解的caspase-1和caspase-11的表达量也有所降低。网络药理学分析表明,诺达凯宁对结肠炎的抑制作用与 PI3K/Akt 通路有关。在结肠类器官模型和小鼠结肠炎模型中,去甲斑蝥素都能有效抑制PI3K/Akt通路的激活,而PI3K/Akt通路激活剂IGF-1的应用则强烈减弱了去甲斑蝥素对肠上皮细胞脓毒症和肠屏障功能障碍的保护作用:结论:Nodakenin至少部分通过抑制PI3K/Akt信号传导来减少肠上皮细胞的脓毒血症,从而保护肠屏障功能并缓解小鼠的CD样结肠炎。Objectives: To investigate the therapeutic mechanism of nodakenin for Crohn's disease (CD)-like colitis in mice.
Methods: Using a colonic organoid model with lipopolysaccharide (LPS)- and ATP-induced pyroptosis, we investigated the effects of nodakenin on pyroptosis, intestinal barrier function and inflammatory response by detecting key pyroptosis-regulating factors and assessing changes in permeability and pro-inflammatory factors. In a mouse model of 2,4,6-trinitrobenzenesulfonic acid (TNBS)-induced CD-like colitis, the therapeutic effect of nodakenin was evaluated by measuring changes in body weight, DAI score, colonic histopathologies, inflammation score, intestinal barrier function and intestinal epithelial cell pyroptosis. The mechanism of nodakenin protection against pyroptosis of intestinal epithelial cells was explored using network pharmacology analysis and in vivo and in vitro experiments.
Results: In LPS- and ATP-induced colonic organoids, treatment with nodakenin significantly inhibited the expressions of NLRP3, GSDMD-N, cleaved caspase-1 and caspase-11, improved intestinal FITC-dextran (FD4, 4000) permeability, and decreased the levels of IL-1β and IL-18. In the mouse model of TNBS-induced colitis, nodakenin treatment significantly alleviated weight loss, reduced DAI score, inflammatory cell infiltration and inflammation score, and decreased serum FD4 and I-FABP levels and bacteria translocation to the mesenteric lymph nodes, spleen and liver. The mice with nodakenin treatment had also lowered expressions of NLRP3, GSDMD-N, cleaved caspase-1 and caspase-11 in the intestinal mucosa. Network pharmacology analysis suggested that the inhibitory effect of nodakenin on colitis was associated with the PI3K/Akt pathway. In both the colonic organoid model and mouse models of colitis, nodakenin effectively inhibited the activation of the PI3K/Akt pathway, and the application of IGF-1, a PI3K/Akt pathway activator, strongly attenuated the protective effect of nodakenin against intestinal epithelial cell pyroptosis and intestinal barrier dysfunction.
Conclusions: Nodakenin protects intestinal barrier function and alleviates CD-like colitis in mice at least partly by inhibiting PI3K/Akt signaling to reduce intestinal epithelial cell pyroptosis.
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