Guangdong Provincial Key Laboratory of Gastroenterology, Department of Gastroenterology, Nanfang Hospital, Southern Medical University, Guangzhou, China.
Department of Hepatobiliary Surgery, Nanfang Hospital, Southern Medical University, Guangzhou, China.
Cell Death Dis. 2014 Jan 16;5(1):e1006. doi: 10.1038/cddis.2013.542.
Advanced oxidation protein products (AOPPs), a novel protein marker of oxidative damage, have been confirmed to accumulate in patients with inflammatory bowel disease (IBD), as well as those with diabetes and chronic kidney disease. However, the role of AOPPs in the intestinal epithelium remains unclear. This study was designed to investigate whether AOPPs have an effect on intestinal epithelial cell (IEC) death and intestinal injury. Immortalized rat intestinal epithelial (IEC-6) cells and normal Sprague Dawley rats were treated with AOPP-albumin prepared by incubation of rat serum albumin (RSA) with hypochlorous acid. Epithelial cell death, nicotinamide adenine dinucleotide phosphate (NADPH) oxidase subunit activity, reactive oxygen species (ROS) generation, apoptosis-related protein expression, and c-jun N-terminal kinase (JNK) phosphorylation were detected both in vivo and in vitro. In addition, we measured AOPPs deposition and IEC death in 23 subjects with Crohn's disease (CD). Extracellular AOPP-RSA accumulation induced apoptosis in IEC-6 cultures. The triggering effect of AOPPs was mainly mediated by a redox-dependent pathway, including NADPH oxidase-derived ROS generation, JNK phosphorylation, and poly (ADP-ribose) polymerase-1 (PARP-1) activation. Chronic AOPP-RSA administration to normal rats resulted in AOPPs deposition in the villous epithelial cells and in inflammatory cells in the lamina propria. These changes were companied with IEC death, inflammatory cellular infiltration, and intestinal injury. Both cell death and intestinal injury were ameliorated by chronic treatment with apocynin. Furthermore, AOPPs deposition was also observed in IECs and inflammatory cells in the lamina propria of patients with CD. The high immunoreactive score of AOPPs showed increased apoptosis. Our results demonstrate that AOPPs trigger IEC death and intestinal tissue injury via a redox-mediated pathway. These data suggest that AOPPs may represent a novel pathogenic factor that contributes to IBD progression. Targeting AOPP-induced cellular mechanisms might emerge as a promising therapeutic option for patients with IBD.
晚期氧化蛋白产物 (AOPPs) 是一种新型氧化损伤蛋白标志物,已被证实在炎症性肠病 (IBD) 患者以及糖尿病和慢性肾脏病患者中积累。然而,AOPPs 在肠道上皮细胞中的作用尚不清楚。本研究旨在探讨 AOPPs 是否对肠道上皮细胞 (IEC) 死亡和肠道损伤有影响。用次氯酸孵育大鼠血清白蛋白 (RSA) 制备 AOPP-白蛋白,处理永生化大鼠肠道上皮 (IEC-6) 细胞和正常 Sprague Dawley 大鼠。体内和体外检测上皮细胞死亡、烟酰胺腺嘌呤二核苷酸磷酸 (NADPH) 氧化酶亚基活性、活性氧 (ROS) 生成、凋亡相关蛋白表达和 c-jun N-末端激酶 (JNK) 磷酸化。此外,我们还测量了 23 例克罗恩病 (CD) 患者的 AOPPs 沉积和 IEC 死亡。细胞外 AOPP-RSA 积累诱导 IEC-6 培养物凋亡。AOPPs 的触发作用主要通过依赖氧化还原的途径介导,包括 NADPH 氧化酶衍生的 ROS 生成、JNK 磷酸化和多聚 (ADP-核糖) 聚合酶-1 (PARP-1) 激活。慢性给予正常大鼠 AOPP-RSA 导致绒毛上皮细胞和固有层炎症细胞中 AOPPs 沉积。这些变化伴随着 IEC 死亡、炎症细胞浸润和肠道损伤。慢性给予 apocynin 可改善细胞死亡和肠道损伤。此外,CD 患者的 IEC 和固有层炎症细胞中也观察到 AOPPs 沉积。AOPPs 的高免疫反应性评分显示凋亡增加。我们的结果表明,AOPPs 通过氧化还原介导的途径触发 IEC 死亡和肠道组织损伤。这些数据表明,AOPPs 可能代表一种新的致病因素,有助于 IBD 的进展。针对 AOPP 诱导的细胞机制可能成为治疗 IBD 患者的一种有前途的治疗选择。
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