抑制 PU.1 可改善代谢功能障碍和非酒精性脂肪性肝炎。
Inhibition of PU.1 ameliorates metabolic dysfunction and non-alcoholic steatohepatitis.
机构信息
Naomi Berrie Diabetes Center, Department of Pathology and Cell Biology, College of Physicians and Surgeons, Columbia University, New York, 10032, USA; State Key Laboratory of Proteomics, Beijing Proteome Research Center, Beijing Institute of Lifeomics, National Center for Protein Sciences (The PHOENIX Center at Beijing), Beijing 102206, China.
Naomi Berrie Diabetes Center, Department of Medicine, College of Physicians and Surgeons, Columbia University, New York, New York, 10032, USA.
出版信息
J Hepatol. 2020 Aug;73(2):361-370. doi: 10.1016/j.jhep.2020.02.025. Epub 2020 Mar 3.
BACKGROUND & AIMS: Obesity is a well-established risk factor for type 2 diabetes (T2D) and non-alcoholic steatohepatitis (NASH), but the underlying mechanisms remain incompletely understood. Herein, we aimed to identify novel pathogenic factors (and possible therapeutic targets) underlying metabolic dysfunction in the liver.
METHODS
We applied a tandem quantitative proteomics strategy to enrich and identify transcription factors (TFs) induced in the obese liver. We used flow cytometry of liver cells to analyze the source of the induced TFs. We employed conditional knockout mice, shRNA, and small-molecule inhibitors to test the metabolic consequences of the induction of identified TFs. Finally, we validated mouse data in patient liver biopsies.
RESULTS
We identified PU.1/SPI1, the master hematopoietic regulator, as one of the most upregulated TFs in livers from diet-induced obese (DIO) and genetically obese (db/db) mice. Targeting PU.1 in the whole liver, but not hepatocytes alone, significantly improved glucose homeostasis and suppressed liver inflammation. Consistently, treatment with the PU.1 inhibitor DB1976 markedly reduced inflammation and improved glucose homeostasis and dyslipidemia in DIO mice, and strongly suppressed glucose intolerance, liver steatosis, inflammation, and fibrosis in a dietary NASH mouse model. Furthermore, hepatic PU.1 expression was positively correlated with insulin resistance and inflammation in liver biopsies from patients.
CONCLUSIONS
These data suggest that the elevated hematopoietic factor PU.1 promotes liver metabolic dysfunction, and may be a useful therapeutic target for obesity, insulin resistance/T2D, and NASH.
LAY SUMMARY
Expression of the immune regulator PU.1 is increased in livers of obese mice and people. Blocking PU.1 improved glucose homeostasis, and reduced liver steatosis, inflammation and fibrosis in mouse models of non-alcoholic steatohepatitis. Inhibition of PU.1 is thus a potential therapeutic strategy for treating obesity-associated liver dysfunction and metabolic diseases.
背景与目的
肥胖是 2 型糖尿病(T2D)和非酒精性脂肪性肝炎(NASH)的一个既定危险因素,但潜在机制仍不完全清楚。在此,我们旨在确定肝脏代谢功能障碍的新发病机制(和可能的治疗靶点)。
方法
我们应用串联定量蛋白质组学策略来富集和鉴定肥胖肝脏中诱导的转录因子(TFs)。我们使用肝细胞的流式细胞术分析诱导 TF 的来源。我们使用条件性敲除小鼠、shRNA 和小分子抑制剂来测试鉴定的 TF 诱导的代谢后果。最后,我们在患者肝活检中验证了小鼠数据。
结果
我们确定了 PU.1/SPI1,一种主要的造血调节因子,是饮食诱导肥胖(DIO)和遗传肥胖(db/db)小鼠肝脏中上调最明显的 TF 之一。靶向整个肝脏中的 PU.1,但不是仅靶向肝细胞,可显著改善葡萄糖稳态并抑制肝脏炎症。一致地,用 PU.1 抑制剂 DB1976 治疗可显著减轻 DIO 小鼠的炎症,改善葡萄糖稳态和血脂异常,并强烈抑制饮食性 NASH 小鼠模型中的葡萄糖不耐受、肝脂肪变性、炎症和纤维化。此外,肝 PU.1 表达与肝活检中患者的胰岛素抵抗和炎症呈正相关。
结论
这些数据表明,升高的造血因子 PU.1 促进肝脏代谢功能障碍,可能是肥胖、胰岛素抵抗/T2D 和 NASH 的有用治疗靶点。
平铺直叙
肥胖小鼠和人类肝脏中免疫调节因子 PU.1 的表达增加。阻断 PU.1 可改善葡萄糖稳态,并减少非酒精性脂肪性肝炎小鼠模型中的肝脂肪变性、炎症和纤维化。因此,抑制 PU.1 可能是治疗肥胖相关肝功能障碍和代谢疾病的潜在治疗策略。
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