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首页> 外文期刊>Journal of biomedical nanotechnology >Development and evaluation of tocopherol-rich argan oil-based nanoemulsions as vehicles possessing anticancer activity
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Development and evaluation of tocopherol-rich argan oil-based nanoemulsions as vehicles possessing anticancer activity

机译:具有抗癌活性的富含生育酚的摩洛哥坚果油基纳米乳液的开发与评价

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In recent years, diverse nanoemulsion vehicles (NEs) have been developed with vast potential for improving therapeutic index of clinically approved and experimental drugs. Using oils rich in omega-3 and omega-6 polyunsaturated fatty acids (PUFA), several promising nanoemulsion formulations have been developed recently for oral and systemic administration. The aim of our present work is to successfully develop and characterize optimized nanoemulsion platform, using the PUFArich argan oil that contain several important anti-inflammatory and antimitotic natural components. Using various emulsifying mixtures of polyethoxylated solutol HS-15 and polyethyleneglucol Vitamin E succinyl ester (TPGS), to form different NEs showing extended shelf-life stability. The physicochemical properties of prototype argan NEs were analyzed and utilizing a 3 ~2 full factorial design, followed by biocompatibility screen, using normal vascular myocytes and areolar fibroblasts. While 90-180 day stability of NEs correlated with TPGS:solutol surfactant blend ratios, adverse effects on integrity of test cultures were only noted at high TPGS content in the emulsifier system, exceeding 80%. Finally, the anti-proliferative efficacy of selected stable and acceptably biocompatible nanoscale TPGS-emulsified argan oil formulations was investigated using murine breast and colon carcinoma cells. The IC50 values of the combination of argan oil and TPGS (40-80%wt of emulsifiers) were 5-9 folds lower compared to TPGS-free and argan-oil free control NEs. Argan oil NE, stabilized with Vitamin E TPGS and solutol HS mixtures, demonstrated significant pro-apoptotic effect on both test cancer cell lines, indicating built-in anticancer properties for such NE platform, potentially enhancing overall antineoplastic effects of incorporated candidate chemotherapeutic agents.
机译:近年来,已经开发了多种纳米乳剂(NEs),它们具有极大的潜力来改善临床批准和实验药物的治疗指数。使用富含omega-3和omega-6多不饱和脂肪酸(PUFA)的油,最近已经开发出几种有前途的纳米乳剂,用于口服和全身给药。我们当前工作的目的是,使用含有多种重要抗炎和抗有丝分裂天然成分的PUFArich摩洛哥坚果油,成功开发和表征优化的纳米乳液平台。使用聚乙氧基化溶胶醇HS-15和聚乙二醇葡萄糖维生素E琥珀酸酯(TPGS)的各种乳化混合物,可形成显示延长的货架期稳定性的不同NE。分析了原型摩洛哥坚果NEs的理化特性,并使用3〜2全因子设计,然后使用正常的血管肌细胞和乳晕成纤维细胞进行生物相容性筛选。尽管NEs的90-180天稳定性与TPGS:solutol表面活性剂的混合比例相关,但只有在乳化剂系统中TPGS含量高(超过80%)时,才对测试培养物的完整性产生不利影响。最后,使用鼠类乳腺癌和结肠癌细胞研究了选定的稳定且可接受的生物相容性纳米级TPGS乳化的摩洛哥坚果油制剂的抗增殖功效。与不含TPGS和不含摩洛哥坚果油的对照NE相比,摩洛哥坚果油和TPGS(40-80%wt的乳化剂)组合的IC50值低5-9倍。用维生素E TPGS和solutol HS混合物稳定的摩洛哥坚果油NE对两种测试癌细胞系均显示出显着的促凋亡作用,表明此类NE平台具有内在的抗癌特性,从而有可能增强所掺入的候选化学治疗剂的总体抗肿瘤作用。

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