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中国精品科技期刊2020
紫杉醇-五味子乙素微乳抗肿瘤作用的研究[J]. 食品工业科技, 2012, (20): 125-128. DOI: 10.13386/j.issn1002-0306.2012.20.005
引用本文: 紫杉醇-五味子乙素微乳抗肿瘤作用的研究[J]. 食品工业科技, 2012, (20): 125-128. DOI: 10.13386/j.issn1002-0306.2012.20.005
Study on preparartion and anti-tumor effect of paclitaxel-schisandrin B microemulsion[J]. Science and Technology of Food Industry, 2012, (20): 125-128. DOI: 10.13386/j.issn1002-0306.2012.20.005
Citation: Study on preparartion and anti-tumor effect of paclitaxel-schisandrin B microemulsion[J]. Science and Technology of Food Industry, 2012, (20): 125-128. DOI: 10.13386/j.issn1002-0306.2012.20.005

紫杉醇-五味子乙素微乳抗肿瘤作用的研究

Study on preparartion and anti-tumor effect of paclitaxel-schisandrin B microemulsion

  • 摘要: 制备紫杉醇-五味子乙素微乳(Paclitaxel-Schisandrin B microemulsions,PSM),评价其稳定性、急性毒性和抗肿瘤作用。利用激光粒度及Zeta电位分布测定仪和SephadexG50色谱柱,测定了PSM的粒径为(98.2±12.6)nm、Zeta电位为(-29.6±5.8)mv和对紫杉醇运载率可达98.2%±0.5%(n=3)。在冷藏(7℃)避光条件下保存1年,粒度、药物运载率几乎无改变。通过比较PSM与紫杉醇的毒性及使用S180肉瘤动物模型,发现与游离紫杉醇相比,PSM显著提高了紫杉醇的抗肿瘤作用,同时显著减轻了紫杉醇的急性毒性。由此可推测PSM有可能成为一种优于紫杉醇注射剂的抗肿瘤药物,抗肿瘤作用更强同时毒性显著减轻。 

     

    Abstract: To prepare paclitaxel-schisandrin B microemulsions containing paclitaxel (Paclitaxel-Schisandrin B microemulsions, PSM) and assess the stability, acute toxicity and anti-tumor activity of PSM.PSM was prepared using polyethylene glycol-two stearoyl acyl phosphatidylethanolamine (PEG-DSPE) , oleic acid, schisandrin B and paclitaxel.The particle size distribution and Zeta potential of PSM were determined using laser particle /Zeta potential analyzer while the loading function of PSM was with the use of Sephadex G50 column.PSM was kept in the cold (7℃) and dark place for 1 year, and then the changes of PSM in its particle size and paclitaxel content were measured to study of its stability.The acute toxicity of PSM was evaluated by comparisons of the acute toxicity of paclitaxel and PSM.The anti-tumor activity of PSM was studied using S180 animal sarcoma model.The diameter, Zeta potential and drug loading efficiency of PSM were (98.2± 12.6) nm, (-29.6±5.8) mv, 98.2%±0.5% (n=3) , respectively.Kept for one year, there was no significant change in the particle size of PSM while the paclitaxel content of PSM was decreased to 91.8% of its original amount, no more than 10%.After intravenous injection, the anti-tumor activity of PSM was enhanced visibly compared with the free paclitaxel however the acute toxicity of PSM was much lower than the free paclitaxel.PSM might become a better anticancer medicine than paclitaxel injection.

     

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