游离脂肪酸抑制AMPK信号通路促进小鼠巨噬细胞葡萄糖酵解和M1极化

doi:10.20039/j.cnki.10073949.2023.03.004

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游离脂肪酸抑制AMPK信号通路促进小鼠巨噬细胞葡萄糖酵解和M1极化
DOI:
                        10.20039/j.cnki.10073949.2023.03.004
                    
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作者单位:(北京医院 国家老年医学中心 国家卫生健康委北京老年医学研究所 国家卫生健康委北京老年医学重点实验室 中国医学科学院老年医学研究院,北京市 100730)
作者简介:左惠演,硕士研究生,主要研究方向为非酒精性脂肪性肝病的发病机制,E-mail:zuohy85@126.com。通信作者窦琳,博士,副研究员,硕士研究生导师,主要研究方向为非酒精性脂肪性肝病和动脉粥样硬化的发病机制,E-mail:doulin4623@bjhmoh.cn。
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基金项目:国家自然科学基金项目(81600618、81770858和81770228)；北京市自然科学基金项目(7182144)

Free fatty acid promotes glycolysis and M1 polarization via inhibiting AMPK pathway in mouse macrophages

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Beijing Hospital & National Geriatrics Center & Beijing Institute of Geriatrics of the National Health Commission & Beijing Key Laboratory of Geriatrics of the National Health Commission & Institute of Geriatrics of the Chinese Academy of Medical Sciences, Beijing 100730, China)

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目的]探讨游离脂肪酸对小鼠巨噬细胞葡萄糖酵解和M1极化的影响,从巨噬细胞代谢重编程和M1极化阐明非酒精性脂肪性肝炎(NASH)的发病机制,为NASH的防治提供新的思路。 [方法]以油酸/棕榈酸(O/P)处理RAW264.7细胞建立游离脂肪酸处理巨噬细胞模型；转染AMP活化蛋白激酶(AMPK)特异siRNA抑制AMPK表达；使用阿卡地新(AICAR)激活AMPK活性。采用qPCR检测巨噬细胞M1型分子标志物(TNF-α、IL-6和MCP-1)、M2型分子标志物(CD206和IL-10)以及葡萄糖酵解相关基因(PGM1、PGK1、GPI1、LDHA、ALDOA、GLUT1和HK2)mRNA水平,采用Western blot检测p-mTOR/mTOR、p-Raptor/Raptor、p-Akt/Akt、p-AMPK和AMPK蛋白水平。 [结果]O/P处理RAW264.7细胞后,p-mTOR/mTOR和p-Akt/Akt蛋白水平升高(P＜0.05),p-Raptor/Raptor、p-AMPK和AMPK蛋白水平降低(P＜0.05),葡萄糖酵解相关基因PGM1、PGK1、GPI1、LDHA、ALDOA、GLUT1和HK2 mRNA水平升高(P＜0.05),促炎因子TNF-α、IL-6和MCP-1 mRNA水平升高(P＜0.05),抑炎因子CD206和IL-10 mRNA水平降低(P＜0.05)。抑制RAW264.7细胞中AMPK表达后,p-mTOR/mTOR和p-Akt/Akt蛋白水平升高(P＜0.05),p-Raptor/Raptor、p-AMPK和AMPK蛋白水平降低(P＜0.05),葡萄糖酵解相关基因PGM1、PGK1、GPI1、LDHA、ALDOA、GLUT1和HK2 mRNA水平升高,促炎因子TNF-α、IL-6和MCP-1 mRNA水平升高(P＜0.05),抑炎因子CD206和IL-10 mRNA水平降低(P＜0.05)。激活AMPK活性可逆转O/P对巨噬细胞葡萄糖酵解和M1极化的影响。 [结论]在RAW264.7细胞中游离脂肪酸通过抑制AMPK信号通路促进葡萄糖酵解和M1型极化。

Abstract:

Aim To explore the effect of free fatty acid on the M1 polarization and glycolysis in mouse macrophages. The mechanism of non-alcoholic steatohepatitis (NASH) pathogenesis is clarified from the perspective of metabolism reprogramming and polarization in macrophages, which will provide a new way for prevention and treatment of NASH. Methods Oleic acid/palmitate acid (O/P) was used to treat RAW264.7 cells to establish cell model. AMPK-specific siRNA was transfected into RAW264.7 cells to knockdown AMPK protein expression. Acadesine (AICAR) was used to stimulate the activation of AMPK. The mRNA levels of M1 type molecular markers (TNF-α, IL-6 and MCP-1), M2 type molecular markers (CD206 and IL-10) and glycolysis related genes (PGM1, PGK1, GPI1, LDHA, ALDOA, GLUT1 and HK2) were detected by qPCR, and the protein levels of p-mTOR/mTOR, p-Raptor/Raptor, p-Akt/Akt, p-AMPK and AMPK were detected by Western blot. Results After treatment of RAW264.7 cells with O/P, the protein levels of p-mTOR/mTOR and p-Akt/Akt increased (P＜0.05), the protein levels of p-Raptor/Raptor, p-AMPK and AMPK decreased (P＜0.05), the mRNA levels of glucose glycolysis related genes PGM1, PGK1, GPI1, LDHA, ALDOA, GLUT1 and HK2 increased (P＜0.05), the mRNA levels of pro-inflammatory factors TNF-α, IL-6 and MCP-1 increased (P＜0.05), while the mRNA levels of anti-inflammatory factors CD206 and IL-10 decreased (P＜0.05). After inhibiting AMPK expression in RAW264.7 cells, the protein levels of p-mTOR/mTOR and p-Akt/Akt increased (P＜0.05), the protein levels of p-Raptor/Raptor, p-AMPK and AMPK decreased (P＜0.05), the mRNA levels of glucose glycolysis related genes PGM1, PGK1, GPI1, LDHA, ALDOA, GLUT1 and HK2 increased (P＜0.05), the mRNA levels of pro-inflammatory factors TNF-α, IL-6 and MCP-1 increased (P＜0.05), while the mRNA levels of anti-inflammatory factors CD206 and IL-10 decreased (P＜0.05). Activation of AMPK activity could reverse the effect of O/P on macrophage polarization and glycolysis. Conclusion Free fatty acid promotes M1 polarization and glycolysis via inhibiting AMPK pathway in mouse macrophages.

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左惠演,黄秀清,沈涛,唐蔚青,马佳睿,徐芳芷,黎健,窦琳.游离脂肪酸抑制AMPK信号通路促进小鼠巨噬细胞葡萄糖酵解和M1极化[J].中国动脉硬化杂志,2023,31(3):205~211.

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收稿日期:2022-06-29
最后修改日期:2022-12-29
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在线发布日期: 2023-03-24

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