PGC-1α抑制M2巨噬细胞极化并减轻肝脏缺血再灌注损伤后的肝纤维化。

PGC-1α inhibits M2 macrophage polarization and alleviates liver fibrosis following hepatic ischemia reperfusion injury.

作者信息

Zhang Yanting, Zhang Linzhong, Zhao Yanmian, He Jing, Zhang Yanghao, Zhang Xiuying

机构信息

Department of Histology and Embryology, School of Basic Medical Sciences, Capital Medical University, Beijing, China.

Department of Gastroenterology, Air Force Medical Center, Beijing, China.

出版信息

Cell Death Discov. 2023 Sep 7;9(1):337. doi: 10.1038/s41420-023-01636-2.

DOI:10.1038/s41420-023-01636-2

PMID:37679346

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC10484946/

Abstract

Oxidative stress can induce inflammation, promoting macrophage polarization and liver fibrosis following hepatic ischemia-reperfusion (I/R). Peroxisome proliferator-activated receptor-γ coactivator-1α (PGC-1α) has anti-oxidant and anti-inflammatory activity. However, how PGC-1α regulates macrophage polarization following hepatic I/R remains largely unknown. Male C57BL/6 wild-type mice were pre-treated with vehicle or trichostatin A (TSA) for 2 days and subjected to surgical induction of I/R. Liver injury and fibrosis in individual mice were examined longitudinally and the expression levels of IL-6, STAT3, M2-type macrophage markers, Collagen I and α-SMA in the liver of mice were analyzed by immunohistochemistry, RT-qPCR and Western blot. The potential interaction of PGC-1α with phosphorylated NF-kBp65 was determined by immunoprecipitation. The impacts of PGC-1α deficiency in hepatocytes on their IL-6 production and macrophage polarization were tested in a Transwell co-culture system. Moreover, the M2-type macrophage polarization and liver fibrosis were examined in hepatocyte-specific PGC-1α knockout mice and AAV8-mediated PGC-1α over-expressing mice following liver I/R. The down-regulated PGC-1α expression by I/R was negatively correlated with IL-6 levels in the liver of I/R mice and PGC-1α deficiency enhanced IL-6 expression, STAT3 activation and M2-type macrophage polarization in the I/R mice, which were abrogated by TSA treatment. In addition, PGC-1α directly interacted with phosphorylated NF-kBp65 in I/R livers. Hepatocyte-specific PGC-1α deficiency increased IL-6 production and promoted macrophage polarization toward M2 type when co-culture. More importantly, administration with AAV8-PGC-1α rescued the I/R-induced liver fibrosis by inhibiting the IL-6/JAK2/STAT3 signaling and M2-type macrophage polarization in the liver. These results suggest that PGC-1α may alleviate the I/R-induced liver fibrosis by attenuating the IL-6/JAK2/STAT3 signaling to limit M2-type macrophage polarization. PGC-1α may be a therapeutic target for the treatment of liver fibrosis.

摘要

氧化应激可诱导炎症，促进肝脏缺血再灌注（I/R）后的巨噬细胞极化和肝纤维化。过氧化物酶体增殖物激活受体γ共激活因子1α（PGC-1α）具有抗氧化和抗炎活性。然而，PGC-1α如何调节肝脏I/R后的巨噬细胞极化仍 largely 未知。雄性C57BL/6野生型小鼠用载体或曲古抑菌素A（TSA）预处理2天，然后进行手术诱导I/R。纵向检查个体小鼠的肝损伤和纤维化，并通过免疫组织化学、RT-qPCR和蛋白质印迹分析小鼠肝脏中IL-6、STAT3、M2型巨噬细胞标志物、胶原蛋白I和α-SMA的表达水平。通过免疫沉淀确定PGC-1α与磷酸化NF-κBp65的潜在相互作用。在Transwell共培养系统中测试肝细胞中PGC-1α缺乏对其IL-6产生和巨噬细胞极化的影响。此外，在肝脏I/R后的肝细胞特异性PGC-1α基因敲除小鼠和AAV8介导的PGC-1α过表达小鼠中检查M2型巨噬细胞极化和肝纤维化。I/R导致的PGC-1α表达下调与I/R小鼠肝脏中的IL-6水平呈负相关，PGC-1α缺乏增强了I/R小鼠中的IL-6表达、STAT3激活和M2型巨噬细胞极化，而TSA处理可消除这些现象。此外，PGC-1α在I/R肝脏中直接与磷酸化NF-κBp65相互作用。肝细胞特异性PGC-1α缺乏增加IL-6产生，并在共培养时促进巨噬细胞向M2型极化。更重要的是，给予AAV8-PGC-1α通过抑制肝脏中的IL-6/JAK2/STAT3信号传导和M2型巨噬细胞极化来挽救I/R诱导的肝纤维化。这些结果表明，PGC-1α可能通过减弱IL-6/JAK2/STAT3信号传导来限制M2型巨噬细胞极化，从而减轻I/R诱导的肝纤维化。PGC-1α可能是治疗肝纤维化的治疗靶点。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/9ee0/10484946/19a939b57e35/41420_2023_1636_Fig1_HTML.jpg

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PGC-1α抑制M2巨噬细胞极化并减轻肝脏缺血再灌注损伤后的肝纤维化。

PGC-1α inhibits M2 macrophage polarization and alleviates liver fibrosis following hepatic ischemia reperfusion injury.

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