ECM1 可防止转化生长因子 β 在小鼠中被激活、肝星状细胞活化以及纤维化形成。
ECM1 Prevents Activation of Transforming Growth Factor β, Hepatic Stellate Cells, and Fibrogenesis in Mice.
机构信息
State Key Laboratory of Cell Biology, CAS Center for Excellence in Molecular Cell Science, Shanghai Institute of Biochemistry and Cell Biology, Chinese Academy of Sciences, University of Chinese Academy of Sciences, Shanghai, China; CAS Key Laboratory of Molecular Virology and Immunology, Institute Pasteur of Shanghai, Shanghai, Chinese Academy of Sciences, University of Chinese Academy of Sciences, Shanghai, China.
Liver Research Center, Beijing Friendship Hospital, Capital Medical University, Beijing, China; Beijing Key Laboratory of Translational Medicine in Liver Cirrhosis and National Clinical Research Center of Digestive Disease, Beijing, China.
出版信息
Gastroenterology. 2019 Nov;157(5):1352-1367.e13. doi: 10.1053/j.gastro.2019.07.036. Epub 2019 Jul 27.
BACKGROUND & AIMS: Activation of TGFB (transforming growth factor β) promotes liver fibrosis by activating hepatic stellate cells (HSCs), but the mechanisms of TGFB activation are not clear. We investigated the role of ECM1 (extracellular matrix protein 1), which interacts with extracellular and structural proteins, in TGFB activation in mouse livers.
METHODS
We performed studies with C57BL/6J mice (controls), ECM1-knockout (ECM1-KO) mice, and mice with hepatocyte-specific knockout of EMC1 (ECM1). ECM1 or soluble TGFBR2 (TGFB receptor 2) were expressed in livers of mice after injection of an adeno-associated virus vector. Liver fibrosis was induced by carbon tetrachloride (CCl) administration. Livers were collected from mice and analyzed by histology, immunohistochemistry, in situ hybridization, and immunofluorescence analyses. Hepatocytes and HSCs were isolated from livers of mice and incubated with ECM1; production of cytokines and activation of reporter genes were quantified. Liver tissues from patients with viral or alcohol-induced hepatitis (with different stages of fibrosis) and individuals with healthy livers were analyzed by immunohistochemistry and in situ hybridization.
RESULTS
ECM1-KO mice spontaneously developed liver fibrosis and died by 2 months of age without significant hepatocyte damage or inflammation. In liver tissues of mice, we found that ECM1 stabilized extracellular matrix-deposited TGFB in its inactive form by interacting with αv integrins to prevent activation of HSCs. In liver tissues from patients and in mice with CCl-induced liver fibrosis, we found an inverse correlation between level of ECM1 and severity of fibrosis. CCl-induced liver fibrosis was accelerated in ECM1 mice compared with control mice. Hepatocytes produced the highest levels of ECM1 in livers of mice. Ectopic expression of ECM1 or soluble TGFBR2 in liver prevented fibrogenesis in ECM1-KO mice and prolonged their survival. Ectopic expression of ECM1 in liver also reduced the severity of CCl-induced fibrosis in mice.
CONCLUSIONS
ECM1, produced by hepatocytes, inhibits activation of TGFB and its activation of HSCs to prevent fibrogenesis in mouse liver. Strategies to increase levels of ECM1 in liver might be developed for treatment of fibrosis.
背景与目的
转化生长因子 β(TGFB)的激活通过激活肝星状细胞(HSCs)促进肝纤维化,但 TGFB 激活的机制尚不清楚。我们研究了细胞外基质蛋白 1(ECM1)在小鼠肝脏 TGFB 激活中的作用,ECM1 与细胞外和结构蛋白相互作用。
方法
我们使用 C57BL/6J 小鼠(对照组)、ECM1 敲除(ECM1-KO)小鼠和肝细胞特异性敲除 ECM1(ECM1)的小鼠进行研究。在注射腺相关病毒载体后,在小鼠肝脏中表达 ECM1 或可溶性 TGFBR2(TGFB 受体 2)。用四氯化碳(CCl)给药诱导肝纤维化。从小鼠中收集肝脏,并通过组织学、免疫组织化学、原位杂交和免疫荧光分析进行分析。从小鼠肝脏中分离出肝细胞和 HSCs 并与 ECM1 孵育;量化细胞因子的产生和报告基因的激活。通过免疫组织化学和原位杂交分析来自病毒性或酒精性肝炎患者(纤维化不同阶段)和健康个体的肝组织。
结果
ECM1-KO 小鼠自发地发生肝纤维化,并在 2 个月大时因无明显的肝细胞损伤或炎症而死亡。在小鼠的肝组织中,我们发现 ECM1 通过与αv 整合素相互作用稳定沉积在细胞外基质中的 TGFB,使其处于无活性形式,从而防止 HSCs 的激活。在患者的肝组织和 CCl 诱导的肝纤维化小鼠中,我们发现 ECM1 的水平与纤维化的严重程度呈负相关。与对照小鼠相比,CCl 诱导的肝纤维化在 ECM1 小鼠中加速。在小鼠的肝脏中,肝细胞产生 ECM1 的水平最高。在 ECM1-KO 小鼠中异位表达 ECM1 或可溶性 TGFBR2 可预防纤维化并延长其存活时间。在小鼠肝脏中异位表达 ECM1 也降低了 CCl 诱导的纤维化的严重程度。
结论
由肝细胞产生的 ECM1 抑制 TGFB 的激活及其对 HSCs 的激活,从而防止小鼠肝脏纤维化。增加 ECM1 在肝脏中的水平的策略可能被开发用于治疗纤维化。
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