细胞珠蛋白缺乏通过激活氧化应激途径,促进从肝脂肪变性发展为肝癌。
Cytoglobin deficiency promotes liver cancer development from hepatosteatosis through activation of the oxidative stress pathway.
作者信息
Thuy Le Thi Thanh, Matsumoto Yoshinari, Thuy Tuong Thi Van, Hai Hoang, Suoh Maito, Urahara Yuka, Motoyama Hiroyuki, Fujii Hideki, Tamori Akihiro, Kubo Shoji, Takemura Shigekazu, Morita Takashi, Yoshizato Katsutoshi, Kawada Norifumi
机构信息
Department of Hepatology, Graduate School of Medicine, Osaka City University, Osaka, Japan.
Department of Hepatology, Graduate School of Medicine, Osaka City University, Osaka, Japan; Department of Medical Nutrition, Graduate School of Human Life Science, Osaka City University, Osaka, Japan.
出版信息
Am J Pathol. 2015 Apr;185(4):1045-60. doi: 10.1016/j.ajpath.2014.12.017. Epub 2015 Feb 7.
This study was conducted to clarify the role of cytoglobin (Cygb), a globin expressed in hepatic stellate cells (HSCs), in the development of liver fibrosis and cancer in nonalcoholic steatohepatitis (NASH). Cygb expression was assessed in patients with NASH and hepatocellular carcinoma. Mouse NASH model was generated in Cygb-deficient (Cygb(-/-)) or wild-type (WT) mice by giving a choline-deficient amino acid-defined diet and, in some of them, macrophage deletion and N-acetyl cysteine treatment were used. Primary-cultured mouse HSCs isolated from WT (HSCs(Cygb-wild)) or Cygb(-/-) (HSCs(Cygb-null)) mice were characterized. As results, the expression of CYGB was reduced in patients with NASH and hepatocellular carcinoma. Choline-deficient amino acid treatment for 8 weeks induced prominent inflammation and fibrosis in Cygb(-/-) mice, which was inhibited by macrophage deletion. Surprisingly, at 32 weeks, despite no tumor formation in the WT mice, all Cygb(-/-) mice developed liver cancer, which was ameliorated by N-acetyl cysteine treatment. Altered expression of 31 genes involved in the metabolism of reactive oxygen species was notable in Cygb(-/-) mice. Both HSCs(Cygb-null) and Cygb siRNA-transfected-HSCs(Cygb-wild) exhibited the preactivation condition. Our findings provide important insights into the role that Cygb, expressed in HSCs during liver fibrosis, plays in cancer development with NASH.
本研究旨在阐明细胞珠蛋白(Cygb),一种在肝星状细胞(HSC)中表达的珠蛋白,在非酒精性脂肪性肝炎(NASH)的肝纤维化和癌症发展中的作用。在NASH患者和肝细胞癌患者中评估了Cygb的表达。通过给予胆碱缺乏氨基酸限定饮食,在Cygb缺陷(Cygb(-/-))或野生型(WT)小鼠中建立小鼠NASH模型,并且在其中一些小鼠中,采用了巨噬细胞缺失和N-乙酰半胱氨酸治疗。对从WT(HSCs(Cygb-wild))或Cygb(-/-)(HSCs(Cygb-null))小鼠分离的原代培养小鼠HSC进行了表征。结果显示,NASH患者和肝细胞癌患者中CYGB的表达降低。对Cygb(-/-)小鼠进行8周的胆碱缺乏氨基酸治疗诱导了显著的炎症和纤维化,巨噬细胞缺失可抑制这种炎症和纤维化。令人惊讶的是,在32周时,尽管WT小鼠未形成肿瘤,但所有Cygb(-/-)小鼠都发生了肝癌,N-乙酰半胱氨酸治疗可改善这种情况。在Cygb(-/-)小鼠中,参与活性氧代谢的31个基因的表达发生了明显改变。HSCs(Cygb-null)和Cygb siRNA转染的HSCs(Cygb-wild)均表现出预激活状态。我们的研究结果为肝纤维化期间在HSC中表达的Cygb在NASH癌症发展中所起的作用提供了重要见解。
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