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Pharmacokinetics and antitumor efficacy of paclitaxel-cyclodextrin complexes loaded in mucus-penetrating nanoparticles for oral administration

机译:紫杉醇-环糊精配合物在穿透黏液的纳米颗粒中的药代动力学和抗肿瘤功效

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摘要

The authors report a novel approach for enhancing the oral absorption of paclitaxel (PTX) by encapsulation in poly(anhydride) nanoparticles (NPs) containing cyclodextrins and poly(ethylene glycol). Materials & methods: Formulations were prepared using the solvent displacement method. Subsequently, pharmacokinetics and organ distribution assays were evaluated after oral administration into C57BL/6J mice. In addition, antitumor efficacy studies were performed in a subcutaneous tumor model of Lewis lung carcinoma. Results: PTX-loaded NPs displayed sizes between 190–300 nm. Oral NPs achieved drug plasma levels for at least 24 h, with an oral bioavailability of 55–80%. Organ distribution studies revealed that PTX, orally administered in NPs, underwent a similar distribution to intravenous Taxol® (Bristol-Myers-Squibb, NJ, USA). For in vivo antitumor assays, oral strategy maintained a slower tumor growth than intravenous Taxol. Conclusion: PTX orally administered in poly(anhydride) NPs, combined with cyclodextrins and poly(ethylene glycol), displayed sustained plasma levels and significant antitumor effect in a syngenic tumor model of carcinoma in mice.
机译:作者报告了一种通过封装在含有环糊精和聚乙二醇的聚(酸酐)纳米颗粒(NP)中来增强紫杉醇(PTX)口服吸收的新方法。材料与方法:使用溶剂置换法制备制剂。随后,在口服给药至C57BL / 6J小鼠后评估了药代动力学和器官分布测定。另外,在路易斯肺癌的皮下肿瘤模型中进行了抗肿瘤功效研究。结果:装载PTX的NP的尺寸在190–300 nm之间。口服NP至少在24 h内达到药物血浆水平,口服生物利用度为55–80%。器官分布研究表明,NPs口服给药的PTX与静脉注射Taxol®(Bristol-Myers-Squibb,美国新泽西州)的分布相似。对于体内抗肿瘤测定,口服策略比静脉内紫杉醇维持较慢的肿瘤生长。结论:在聚(酸酐)NPs中口服PTX,与环糊精和聚(乙二醇)结合,在小鼠的同基因肿瘤模型中显示持续的血浆水平和显着的抗肿瘤作用。

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