自噬
ABCG1公司
肝X受体
ABCA1
安普克
泡沫电池
芒果苷
胆固醇
下调和上调
巨噬细胞
胆固醇逆向转运
化学
药理学
PI3K/AKT/mTOR通路
内科学
细胞生物学
脂蛋白
医学
生物
生物化学
信号转导
激酶
蛋白激酶A
细胞凋亡
体外
运输机
核受体
基因
转录因子
作者
Qian Chen,Sijian Wang,Ruixia Bao,Dan Wang,Yuzheng Wu,Yi Zhang,Mengyang Liu,Tao Wang
标识
DOI:10.1186/s13020-023-00876-9
摘要
BACKGROUND: The synthetic liver X receptor ligand (LXR) T0901317 (T0) has been reported to attenuate atherosclerosis (AS) without hyperglyceridemia due to innovative drug combination or nano-sized drug delivery. Given the key roles of mangiferin (MGF) in lipid metabolism and atherogenesis, it is critical to investigate progression of atherosclerotic lesion after combined treatment of MGF and T0. METHODS: mice among T0 and/or MGF treatment. The in vitro functions of MGF and T0 were analyzed by Oil-red O staining, cholesterol efflux assay, transmission electron microscopy and western blot analyses with or without acetylated low density lipoprotein. RESULTS: mice, due to upregulation of ABCA1 and ABCG1 induced by LXR activation. Subsequently, we identified autophagy promoted by MGF and T0 treatment establishes a positive feedback loop that increases cholesterol efflux, resulted from LXRα activation. Under atherogenic conditions, the autophagy inhibitor CQ abolished the enhancement effect on cholesterol outflow of MGF and T0. Mechanically, MGF and T0 promotes LXRα and mTOR/AMPK signaling cascade in macrophage, and promotes AMPK signaling cascade in hepatocyte, leading to lipid metabolic homeostasis. CONCLUSIONS: Altogether, our findings reveal that MGF and T0 engages in AS therapy without side effects by activating AMPK-dependent autophagy to promote macrophage cholesterol efflux, and MGF might serve as a natural compound to assist T0 in AS via targeting autophagy.
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