肝靶向纳米颗粒GA-MSe@AR通过双重降脂和抗氧化功效治疗非酒精性脂肪性肝病
Liver-Targeting Nanoparticles GA-MSe@AR Treat NAFLD Through Dual Lipid-Lowering and Antioxidant Efficacy.
作者信息
Lei Sheng, Wu Qiang, Zhang Bin, Lu Minqiang, Xia Yu, Li Ning
机构信息
Department of HBP Surgery, The Second Affiliated Hospital, School of Medicine, South China University of Technology, Guangzhou, 510180, People's Republic of China.
Department of Gastroenterology and Hepatology, Guangzhou Digestive Disease Center, The Second Affiliated Hospital, School of Medicine, South China University of Technology, Guangzhou, 510180, People's Republic of China.
出版信息
Int J Nanomedicine. 2025 Apr 18;20:5017-5037. doi: 10.2147/IJN.S510577. eCollection 2025.
BACKGROUND AND PURPOSE
Non-alcoholic fatty liver disease (NAFLD) is prevalent worldwide and lacks effective treatments. Arctiin (AR), a natural product, has shown promise for NAFLD therapy, due to its antioxidant, anti-inflammatory, and inhibition adipogenesis properties. However, its therapeutic efficacy is hindered by low water solubility, poor bioavailability, and inadequate liver targeting. In this study, selenium-based antioxidant nanoparticles were developed to load and deliver AR to the liver for synergistic AR and selenium effective treatment of NAFLD.
METHODS
The therapeutic potential of AR was analyzed by network pharmacology. GA-MSe@AR was synthesized by encapsulating AR within galactose-modified mesoporous selenium nanoparticles (GA-MSe) for liver-specific targeting. The nanoparticle size, chemical structure, and elemental composition were explored. The toxicity, cellular uptake, lysosomal escape, and AR release efficiency of GA-MSe@AR were investigated by in vitro experiments. The liver targeting ability of GA-MSe@AR was evaluated through live imaging. The lipid-lowering and antioxidant activities of GA-MSe@AR were assessed in both in vitro and in vivo NAFLD models. Additionally, its effects on inflammation and pancreatic function were analyzed in vivo.
RESULTS
Network pharmacology analysis revealed AR may against NAFLD through regulating metabolism, inflammation, and oxidative stress. GA-MSe@AR exhibited low toxicity, efficient cellular uptake, remarkable lysosomal escape ability, and high AR release efficiency in vitro. In both in vitro and in vivo NAFLD models, GA-MSe@AR demonstrated more pronounced lipid-lowering and antioxidant properties than AR and GA-MSe. Additionally, GA-MSe@AR effectively targeted the liver, resulting in a greater decrease in blood glucose, lipids, ALT, AST levels, and reduction liver inflammation, as well as improved pancreatic function in high-fat diet (HFD)-fed mice compared to AR alone.
CONCLUSION
The GA-specific modification enhanced liver-targeted accumulation of the selenium-based nanoparticles, enabling precise targeted delivery of AR. GA-MSe@AR demonstrated superior lipid-lowering efficacy and antioxidant activity in a NAFLD mice model. These findings collectively establish GA-MSe@AR as a promising therapeutic candidate for NAFLD treatment.
背景与目的
非酒精性脂肪性肝病(NAFLD)在全球范围内普遍存在且缺乏有效的治疗方法。牛蒡子苷(AR)作为一种天然产物,因其具有抗氧化、抗炎和抑制脂肪生成的特性,在NAFLD治疗方面显示出前景。然而,其低水溶性、低生物利用度和肝脏靶向性不足阻碍了其治疗效果。在本研究中,开发了基于硒的抗氧化纳米颗粒来负载并将AR递送至肝脏,以实现AR与硒协同有效治疗NAFLD。
方法
通过网络药理学分析AR的治疗潜力。通过将AR包裹于半乳糖修饰的介孔硒纳米颗粒(GA-MSe)中以实现肝脏特异性靶向,合成了GA-MSe@AR。探究了纳米颗粒的大小、化学结构和元素组成。通过体外实验研究了GA-MSe@AR的毒性、细胞摄取、溶酶体逃逸和AR释放效率。通过活体成像评估GA-MSe@AR的肝脏靶向能力。在体外和体内NAFLD模型中评估GA-MSe@AR的降脂和抗氧化活性。此外,在体内分析了其对炎症和胰腺功能的影响。
结果
网络药理学分析显示AR可能通过调节代谢、炎症和氧化应激来对抗NAFLD。GA-MSe@AR在体外表现出低毒性、高效的细胞摄取、显著的溶酶体逃逸能力和高AR释放效率。在体外和体内NAFLD模型中,GA-MSe@AR均表现出比AR和GA-MSe更显著的降脂和抗氧化特性。此外,GA-MSe@AR有效地靶向肝脏,与单独使用AR相比,在高脂饮食(HFD)喂养的小鼠中,导致血糖、血脂、谷丙转氨酶(ALT)、谷草转氨酶(AST)水平更大幅度的降低,肝脏炎症减轻,以及胰腺功能改善。
结论
GA特异性修饰增强了基于硒的纳米颗粒在肝脏中的靶向积累,实现了AR的精确靶向递送。GA-MSe@AR在NAFLD小鼠模型中表现出优异的降脂疗效和抗氧化活性。这些发现共同确立了GA-MSe@AR作为NAFLD治疗的一种有前景的治疗候选物。
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