O-GlcNAcylation 依赖性的 HO1 上调触发氨诱导的肝性脑病中的氧化应激和衰老。
O-GlcNAcylation-dependent upregulation of HO1 triggers ammonia-induced oxidative stress and senescence in hepatic encephalopathy.
机构信息
Clinic for Gastroenterology, Hepatology and Infectious Diseases, Heinrich-Heine-University, 40225 Düsseldorf, Germany.
Clinic for Gastroenterology, Hepatology and Infectious Diseases, Heinrich-Heine-University, 40225 Düsseldorf, Germany.
出版信息
J Hepatol. 2019 Nov;71(5):930-941. doi: 10.1016/j.jhep.2019.06.020. Epub 2019 Jul 4.
BACKGROUND & AIMS: Cerebral oxidative stress plays an important role in the pathogenesis of hepatic encephalopathy (HE), but the underlying mechanisms are incompletely understood. Herein, we analyzed a role of heme oxygenase (HO)1, iron and NADPH oxidase 4 (Nox4) for the induction of oxidative stress and senescence in HE.
METHODS
Gene and protein expression in human post-mortem brain samples was analyzed by gene array and western blot analysis. Mechanisms and functional consequences of HO1 upregulation were studied in NHCl-exposed astrocytes in vitro by western blot, qPCR and super-resolution microscopy.
RESULTS
HO1 and the endoplasmic reticulum (ER) stress marker grp78 were upregulated, together with changes in the expression of multiple iron metabolism-related genes, in post-mortem brain samples from patients with liver cirrhosis and HE. NHCl elevated HO1 protein and mRNA in cultured astrocytes through glutamine synthetase (GS)-dependent upregulation of glutamine/fructose amidotransferases 1/2 (GFAT1/2), which blocked the transcription of the HO1-targeting miR326-3p in a O-GlcNAcylation dependent manner. Upregulation of HO1 by NHCl triggered ER stress and was associated with elevated levels of free ferrous iron and expression changes in iron metabolism-related genes, which were largely abolished after knockdown or inhibition of GS, GFAT1/2, HO1 or iron chelation. NHCl, glucosamine (GlcN) and inhibition of miR326-3p upregulated Nox4, while knockdown of Nox4, GS, GFAT1/2, HO1 or iron chelation prevented NHCl-induced RNA oxidation and astrocyte senescence. Elevated levels of grp78 and O-GlcNAcylated proteins were also found in brain samples from patients with liver cirrhosis and HE.
CONCLUSION
The present study identified glucosamine synthesis-dependent protein O-GlcNAcylation as a novel mechanism in the pathogenesis of HE that triggers oxidative and ER stress, as well as senescence, through upregulation of HO1 and Nox4.
LAY SUMMARY
Patients with liver cirrhosis frequently exhibit hyperammonemia and suffer from cognitive and motoric dysfunctions, which at least in part involve premature ageing of the astrocytes in the brain. This study identifies glucosamine and an O-GlcNAcylation-dependent disruption of iron homeostasis as novel triggers of oxidative stress, thereby mediating ammonia toxicity in the brain.
背景与目的
脑氧化应激在肝性脑病(HE)发病机制中起重要作用,但其中的机制尚不完全清楚。在此,我们分析了血红素加氧酶(HO)1、铁和 NADPH 氧化酶 4(Nox4)在 HE 中诱导氧化应激和衰老中的作用。
方法
通过基因芯片和 Western blot 分析分析了人死后脑组织样本中的基因和蛋白表达。通过 Western blot、qPCR 和超分辨率显微镜研究了 NHCl 暴露的星形胶质细胞中 HO1 上调的机制和功能后果。
结果
肝硬化和 HE 患者死后脑组织样本中 HO1 和内质网(ER)应激标志物 grp78 上调,同时多个铁代谢相关基因的表达发生变化。NHCl 通过谷氨酰胺合成酶(GS)依赖性上调谷氨酰胺/果糖酰胺转移酶 1/2(GFAT1/2)来升高培养的星形胶质细胞中的 HO1 蛋白和 mRNA,从而以 O-GlcNAcylation 依赖的方式阻断 HO1 靶向 miR326-3p 的转录。NHCl 上调 HO1 会引发 ER 应激,并与游离亚铁水平升高和铁代谢相关基因的表达变化相关,而这些变化在 GS、GFAT1/2、HO1 或铁螯合后被大大消除。NHCl、葡萄糖胺(GlcN)和 miR326-3p 抑制可上调 Nox4,而 Nox4、GS、GFAT1/2、HO1 或铁螯合抑制可防止 NHCl 诱导的 RNA 氧化和星形胶质细胞衰老。在肝硬化和 HE 患者的脑样本中也发现了 grp78 和 O-GlcNAc 化蛋白的水平升高。
结论
本研究确定了葡萄糖胺合成依赖性蛋白 O-GlcNAcylation 是 HE 发病机制中的一种新机制,它通过上调 HO1 和 Nox4 引发氧化和 ER 应激以及衰老。
要点总结
肝硬化患者常出现高氨血症,并伴有认知和运动功能障碍,这至少部分涉及大脑星形胶质细胞的过早衰老。本研究确定了葡萄糖胺和 O-GlcNAc 依赖性铁稳态破坏作为氧化应激的新触发因素,从而介导了脑中的氨毒性。
Zotero 插件