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新型紫杉醇载 PLGA 纳米粒的研制:对前列腺癌细胞的抗增殖活性及其分子相互作用的研究。

Development of innovative paclitaxel-loaded small PLGA nanoparticles: study of their antiproliferative activity and their molecular interactions on prostatic cancer cells.

机构信息

Université Lille Nord de France, F-59000 Lille, France.

出版信息

Int J Pharm. 2013 Oct 1;454(2):712-9. doi: 10.1016/j.ijpharm.2013.05.018. Epub 2013 May 21.

DOI:10.1016/j.ijpharm.2013.05.018
PMID:23707251
Abstract

Taxanes, including paclitaxel, are anti-cancer drugs approved for the treatment of prostate cancer but which have limited clinical application due to their hydrophobicity, their low therapeutic index and the emergence of chemoresistance. These side effects may be avoided through the use of new drug delivery systems such as nanoparticles, and paclitaxel-loaded PLGA nanoparticles up to 200 nm in size have shown encouraging results. As it is known that size affects the tissular penetration and distribution of tumors via the enhanced permeability and retention effect, so nanoparticles smaller than 100 nm are potentially interesting vehicles for improving paclitaxel delivery and efficacy. In this work, new paclitaxel-loaded small PLGA nanoparticles, between 49 nm and 95 nm in size and with positive or negative surface charges, were prepared without detergent. They were stable in the presence of serum, and HPLC showed that high paclitaxel loading and stability were achieved. Intracellular uptake of these nanoparticles was studied in PC3 cells by flow cytometry. Confocal studies confirmed a high tubulin destructuration at very low dose with these nanoparticles. This study suggests that both positively and negatively charged paclitaxel-loaded small PLGA nanoparticles deliver this drug into PC3 cells, and that this nanoparticle mode of delivery highly improves paclitaxel efficiency by up to two log-increase. These results also highlight the importance of small nanoparticles for drug delivery in cancer applications and are extremely promising for in vivo studies.

摘要

紫杉烷类药物,包括紫杉醇,是一种抗癌药物,已被批准用于治疗前列腺癌,但由于其疏水性、治疗指数低以及出现化疗耐药性,其临床应用受到限制。通过使用新的药物传递系统,如纳米粒子,可以避免这些副作用,并且载紫杉醇的 PLGA 纳米粒子的尺寸可达 200nm 时已显示出令人鼓舞的结果。由于众所周知,尺寸通过增强的通透性和保留效应影响肿瘤的组织穿透和分布,因此小于 100nm 的纳米粒子可能是改善紫杉醇传递和疗效的潜在有趣载体。在这项工作中,制备了新的载紫杉醇的小 PLGA 纳米粒子,尺寸在 49nm 至 95nm 之间,具有正或负表面电荷,无需去污剂。它们在存在血清时稳定,HPLC 表明实现了高紫杉醇负载和稳定性。通过流式细胞术研究了这些纳米粒子在 PC3 细胞中的细胞内摄取。共聚焦研究证实,这些纳米粒子以非常低的剂量可高度破坏微管蛋白。这项研究表明,带正电荷和负电荷的载紫杉醇小 PLGA 纳米粒子均可将药物递送至 PC3 细胞,并且这种纳米粒子递药方式可使紫杉醇的效率提高高达两个对数级。这些结果还强调了小纳米粒子在癌症应用中药物传递的重要性,并且对于体内研究极具前景。

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