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中国精品科技期刊2020
王荣荣,钱怡霖,唐智鑫,等. 壳聚糖包覆荷叶碱脂质体的理化表征及其体内降脂作用[J]. 食品工业科技,2023,44(7):1−9. doi: 10.13386/j.issn1002-0306.2022090226.
引用本文: 王荣荣,钱怡霖,唐智鑫,等. 壳聚糖包覆荷叶碱脂质体的理化表征及其体内降脂作用[J]. 食品工业科技,2023,44(7):1−9. doi: 10.13386/j.issn1002-0306.2022090226.
WANG Rongrong, QIAN Yilin, TANG Zhixin, et al. Physicochemical Characterization and in Vivo Hypolipidemic Effect of Chitosan-Coated Nuciferine Liposomes[J]. Science and Technology of Food Industry, 2023, 44(7): 1−9. (in Chinese with English abstract). doi: 10.13386/j.issn1002-0306.2022090226.
Citation: WANG Rongrong, QIAN Yilin, TANG Zhixin, et al. Physicochemical Characterization and in Vivo Hypolipidemic Effect of Chitosan-Coated Nuciferine Liposomes[J]. Science and Technology of Food Industry, 2023, 44(7): 1−9. (in Chinese with English abstract). doi: 10.13386/j.issn1002-0306.2022090226.

壳聚糖包覆荷叶碱脂质体的理化表征及其体内降脂作用

Physicochemical Characterization and in Vivo Hypolipidemic Effect of Chitosan-Coated Nuciferine Liposomes

  • 摘要: 目的:制备壳聚糖包覆荷叶碱脂质体(chitosan-coated nuciferine liposomes,CS-LP)并研究其体内降脂作用。方法:用薄膜分散法和pH梯度法制备壳聚糖包覆荷叶碱脂质体,对其粒径、电位分布、包封率、微观形态和体外释放曲线进行测定,并探究其对肥胖小鼠的降脂作用。结果:制得的CS-LP为均匀球体结构,粒径大小为253.54±4.25 nm,Zeta电位为32.50±3.44 mV,包封率达83.46%。相比荷叶碱脂质体(nuciferine liposomes,LP),外加壳聚糖涂层可以提高其在模拟消化液中的稳定性。与高脂饮食组相比,CS-LP灌胃11周后,小鼠体重和脂肪组织重量分别显著降低了12.91%和41.03%(P<0.05),血清甘油三酯和低密度脂蛋白胆固醇质量浓度分别显著降低了32.40%和14.49%(P<0.05),血脂水平趋向正常,脂肪细胞体积减小。高通量测序显示,CS-LP显著提高了小鼠肠道菌群的多样性(P<0.05)。在门水平上,小鼠肠道菌群厚壁菌门相对丰度下降,杆菌门相对丰度显著上升,弯曲杆菌门和厚壁菌门的比值与拟杆菌门相对丰度显著降低(P<0.05)。结论:壳聚糖包覆荷叶碱脂质体包封率高,缓释性好,可以有效改善高脂饮食导致的小鼠肥胖和肠道菌群紊乱,在降脂配方食品开发中具有广阔的应用前景。

     

    Abstract: Objective: Chitosan-coated nuciferine liposomes (CS-LP) were prepared and their hypolipidemic effects in vivo were investigated. Methods: The CS-LP were prepared by thin film dispersion and pH gradient methods, and their particle size and potential distribution, encapsulation rate, microscopic morphology and in vitro release curves were determined, and their hypolipidemic effects on obese mice were investigated. Results: The CS-LP was produced in a homogeneous spherical structure with a particle size of 253.54±4.25 nm, a zeta potential of 32.50±3.44 mV. The encapsulation rate of CS-LP was 83.46%. Compared with nuciferine liposomes (LP), the stability of CS-LP in the simulated digestive solution was improved after adding the chitosan. Compared with the high-fat group, mice gavaged with CS-LP for 11 weeks showed a 12.91% and 41.03% significant reduction in body weight and adipose tissue weight, respectively (P<0.05), a 32.40% and 14.49% significant reduction in serum triglyceride and LDL cholesterol mass concentrations, respectively (P<0.05), and a normalization of lipid levels and a reduction in adipocyte volume. High-throughput sequencing analysis showed that CS-LP significantly increased the diversity of intestinal flora in mice (P<0.05). At the phylum level, the relative abundance of the thick-walled phylum and the relative abundance of the bacillus phylum increased significantly, and the ratio of the campylobacter and thick-walled phylum to the relative abundance of the mimic phylum also significantly decreased (P<0.05). Conclusion: The chitosan-coated nuciferine liposomes with high encapsulation rate and slow release could effectively improve obesity and intestinal flora disorders in mice caused by high-fat diet, and express the broad application prospects in the development of lipid-lowering formulations.

     

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