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Enhancement of the bioavailability of a novel anticancer compound (acetyltanshinone IIA) by encapsulation within mPEG-PLGA nanoparticles: a study of formulation optimization toxicity and pharmacokinetics

机译:通过封装在mPEG-PLGA纳米颗粒中来增强新型抗癌化合物(乙酰丹参酮IIA)的生物利用度:配方优化毒性和药代动力学的研究

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摘要

The Poly (ethylene glycol) methyl ether-block-poly (lactide-co-glycolide) (mPEG-PLGA) nanoparticles carrying acetyltanshinone IIA (ATA), a novel anti-breast cancer agent, were prepared by ultrasonic emulsion method to enhance the bioavailability and reduce the toxicity. Systematic optimization of encapsulation process was achieved using an orthogonal design. Drug efficacy analysis showed that ATA nanoparticles were as effective as free ATA against estrogen receptor positive breast cancer cells, but much less toxic towards human endothelial cells. Furthermore, in zebrafish, ATA nanoparticles displayed much lower toxicity than free ATA. More importantly, the blood concentration of ATA nanoparticles indicated by 24 hour-area under the curve (AUC0-24h) was 10 times higher than free ATA. These results indicated the potential of ATA-loaded mPEG-PLGA nanoparticles for the delivery of ATA in a clinical formulation, and their potential for use in tumor therapy in the future.
机译:通过超声乳液法制备了载有新型抗乳腺癌药物乙酰丹参酮IIA(ATA)的聚乙二醇乙二醇醚嵌段聚丙交酯乙交酯(mPEG-PLGA)纳米颗粒,以提高其生物利用度。并降低毒性。使用正交设计实现了封装过程的系统优化。药物功效分析表明,ATA纳米颗粒对雌激素受体阳性的乳腺癌细胞与游离ATA一样有效,但对人内皮细胞的毒性要小得多。此外,在斑马鱼中,ATA纳米颗粒的毒性比游离ATA低得多。更重要的是,曲线下的24小时区域(AUC0-24h)表示的ATA纳米颗粒的血液浓度是游离ATA的10倍。这些结果表明,载有ATA的mPEG-PLGA纳米颗粒具有在临床制剂中传递ATA的潜力,以及它们将来在肿瘤治疗中的潜力。

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