Lipid metabolism imbalance combined with over-activated inflammation are two key factors for hepatic stestosis. However, on-demand anchoring inflammation and lipid metabolism disorder for hepatic stestosis treatment has yet to be realized. Here we propose a charge reversal fullerene based nano-assembly to migrate hepatic steatosis via inhibiting macrophage-mediated inflammation and normalizing hepatocellular lipid metabolism in obesity mice. Our nano-assembly (abbreviated as FPPD) is comprised of electropositive polyetherimide (PEI), charge-shielded dimethylmaleic anhydride (DMA), and poly(lactic-co-glycolic acid) (PLGA), which provides hydrophobic chains for self-assembly with anti-oxidative dicarboxy fullerene poly(ethylene glycol) molecule (FP). The obtained FPPD nano-assembly owns a charge reversal ability that switches to a positive charge in an acidic environment that targets the electronegative mitochondria both in pro-inflammatory macrophages and steatosis hepatocytes. We demonstrate that the anti-oxidative and mitochondria-targeting FPPD notably reduces inflammation in macrophages and lipid accumulation in hepatocytes by quenching excessive reactive oxygen species (ROS) and improving mitochondrial function in vitro. Importantly, FPPD nano-assembly reveals a superior anti-hepatic steatosis effect via migrating inflammation and facilitating lipid transport in obesity mice. Overall, the charge reversal nano-assembly reduces over-activated inflammation and promotes lipid metabolism that provides an effectiveness of a multi-target strategy for hepatic steatosis treatment.
A charge reversal nano-assembly prevents hepatic steatosis by resolving inflammation and improving lipid metabolism.
电荷反转纳米组装体通过消除炎症和改善脂质代谢来预防肝脂肪变性
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作者:Wang Haoyu, Su Sheng'e, An Xin, Xu Yuan, Sun Jiacheng, Zhen Mingming, Wang Chunru, Bai Chunli
| 期刊: | Bioactive Materials | 影响因子: | 20.300 |
| 时间: | 2025 | 起止号: | 2024 Dec 5; 45:496-508 |
| doi: | 10.1016/j.bioactmat.2024.11.023 | 研究方向: | 代谢 |
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