RIP3 的缺失引发了高脂肪饮食引发的非酒精性肝脂肪变性的消除:一种涉及 Toll 样受体 4 和氧化应激的机制。
Loss of RIP3 initiates annihilation of high-fat diet initialized nonalcoholic hepatosteatosis: A mechanism involving Toll-like receptor 4 and oxidative stress.
机构信息
Chongqing Key Laboratory of Medicinal Resources in the Three Gorges Reservoir Region, School of Biological and Chemical Engineering, Chongqing University of Education, Chongqing 400067, PR China; Research Center of Brain Intellectual Promotion and Development for Children Aged 0-6 Years, Chongqing University of Education, Chongqing 400067, PR China.
Chongqing Key Laboratory of Medicinal Resources in the Three Gorges Reservoir Region, School of Biological and Chemical Engineering, Chongqing University of Education, Chongqing 400067, PR China; Research Center of Brain Intellectual Promotion and Development for Children Aged 0-6 Years, Chongqing University of Education, Chongqing 400067, PR China.
出版信息
Free Radic Biol Med. 2019 Apr;134:23-41. doi: 10.1016/j.freeradbiomed.2018.12.034. Epub 2018 Dec 30.
Non-alcoholic fatty liver disease (NAFLD) is a prevalent and complex disease that confers a high risk of severe liver disorders. Although such public and clinical health importance, very few effective therapies are presently available for NAFLD. Here, we showed that receptor-interacting kinase-3 (RIP3) was up-regulated in liver of mouse with hepatic steatosis induced by high fat diet (HFD). After 16 weeks on a HFD, obesity, insulin resistance, metabolic syndrome, hepatic steatosis, inflammatory response and oxidative stress were significantly alleviated in liver of mice with the loss of RIP3. We provided mechanistic evidence that RIP3 knockdown attenuated hepatic dyslipidemia through preventing the expression of lipogenesis-associated genes. Furthermore, in the absence of RIP3, the transcription factor of nuclear factor-κB (NF-κB) signaling pathway activated by HFD was blocked, accompanied with the inhibition of NLRP3 inflammasome. We also found that RIP3 knockdown-induced activation of nuclear factor-erythroid 2 related factor 2/heme oxygenase-1 (Nrf-2/HO-1) led to the inhibition of oxidative stress. The detrimental effects of RIP3 on hepatic steatosis and related pathologies were confirmed in palmitate (PAL)-treated mouse liver cells. Of note, lipopolysaccharide (LPS)- or PAL-activated TLR-4 resulted in the up-regulation of RIP3 that was accompanied by the elevated inflammation and lipid deposition, and these effects were reversed in TLR-4 knockdown cells. Furthermore, promoting Nrf-2 pathway activation effectively reduced reactive oxygen species (ROS) generation and RIP3 expression in PAL-stimulated cells, consequently leading to the suppression of cellular inflammation and lipid accumulation. In contrast, blocking Nrf-2/HO-1 signaling abrogated RIP3 knockdown-reduced reactive oxygen species (ROS), inflammatory response and lipid deposition in PAL-stimulated cells. Taken together, the present study helped to elucidate how HFD-induced hepatic steatosis was regulated by RIP3, via the TLR-4/NF-κB and Nrf-2/HO-1 signaling pathways.
非酒精性脂肪性肝病(NAFLD)是一种普遍且复杂的疾病,会增加严重肝脏疾病的风险。尽管具有如此重要的公共和临床健康意义,但目前针对 NAFLD 的有效治疗方法却很少。在这里,我们发现受体相互作用激酶 3(RIP3)在高脂肪饮食(HFD)诱导的肝脂肪变性的小鼠肝脏中上调。在 HFD 喂养 16 周后,RIP3 缺失的小鼠肝脏中肥胖、胰岛素抵抗、代谢综合征、肝脂肪变性、炎症反应和氧化应激明显减轻。我们提供了机制证据表明,RIP3 敲低通过阻止脂肪生成相关基因的表达来减轻肝脂质代谢紊乱。此外,在不存在 RIP3 的情况下,HFD 激活的核因子-κB(NF-κB)信号通路的转录因子被阻断,伴随着 NLRP3 炎性小体的抑制。我们还发现,RIP3 敲低诱导的核因子-红细胞 2 相关因子 2/血红素加氧酶-1(Nrf-2/HO-1)的激活导致氧化应激的抑制。RIP3 对棕榈酸(PAL)处理的小鼠肝细胞中肝脂肪变性及相关病变的有害影响得到了证实。值得注意的是,脂多糖(LPS)或 PAL 激活的 TLR-4 导致 RIP3 的上调,同时伴有炎症和脂质沉积的增加,这些作用在 TLR-4 敲低细胞中得到逆转。此外,促进 Nrf-2 通路的激活可有效减少 PAL 刺激细胞中的活性氧(ROS)生成和 RIP3 表达,从而抑制细胞炎症和脂质堆积。相反,阻断 Nrf-2/HO-1 信号通路会减弱 PAL 刺激细胞中 RIP3 敲低减少的活性氧(ROS)、炎症反应和脂质沉积。总之,本研究有助于阐明 HFD 诱导的肝脂肪变性如何通过 TLR-4/NF-κB 和 Nrf-2/HO-1 信号通路被 RIP3 调控。
Zotero 插件