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基于胶束形成的两亲性或水溶性聚合物-阿霉素缀合物的聚合物纳米药物:与聚合物载体结构、组成和流体力学性质相关的体外和体内性质的比较研究。

Polymer nanomedicines based on micelle-forming amphiphilic or water-soluble polymer-doxorubicin conjugates: Comparative study of in vitro and in vivo properties related to the polymer carrier structure, composition, and hydrodynamic properties.

机构信息

Institute of Macromolecular Chemistry, Czech Academy of Sciences, Heyrovského nám. 2, 162 06 Prague 6, Czech Republic.

Institute of Microbiology, Czech Academy of Sciences, Vídeňská 1083, 142 20 Prague 4, Czech Republic.

出版信息

J Control Release. 2020 May 10;321:718-733. doi: 10.1016/j.jconrel.2020.03.002. Epub 2020 Mar 3.

DOI:10.1016/j.jconrel.2020.03.002
PMID:32142741
Abstract

The study compared the physico-chemical and biological properties of a water-soluble star-like polymer nanomedicine with three micellar nanomedicines formed by self-assembly of amphiphilic copolymers differing in their hydrophobic part (statistical, block and thermosensitive block copolymers). All nanomedicines showed a pH-responsive release of the drug, independent on polymer structure. Significant penetration of all polymer nanomedicines into tumor cells in vitro was demonstrated, where the most pronounced effect was observed for statistical- or diblock copolymer-based micellar systems. Tumor accumulation in vivo was dependent on the stability of the nanomedicines in solution, being the highest for the star-like system, followed by the most stable micellar nanomedicines. The star-like polymer nanomedicine showed a superior therapeutic effect. Since the micellar systems exhibited slightly lower systemic toxicity, they may exhibit the same efficacy as the star-like soluble system when administered at equitoxic doses. In conclusion, treatment efficacy of studied nanomedicines was directly controlled by the drug pharmacokinetics, namely by their ability to circulate in the bloodstream for the time needed for effective accumulation in the tumor due to the enhanced permeability and retention (EPR) effect. Easy and scalable synthesis together with the direct reconstitution possibility for nanomedicine application made these nanomedicines excellent candidates for further clinical evaluation.

摘要

该研究比较了一种水溶性星型聚合物纳米药物与通过自组装形成的三种胶束纳米药物的物理化学和生物学特性,这三种胶束纳米药物由不同疏水部分的两亲性共聚物组成(统计、嵌段和热敏嵌段共聚物)。所有纳米药物均表现出对药物的 pH 响应释放,与聚合物结构无关。研究表明,所有聚合物纳米药物均能显著穿透体外肿瘤细胞,其中统计或嵌段共聚物胶束系统的效果最为明显。体内肿瘤积累取决于纳米药物在溶液中的稳定性,星形系统最高,其次是最稳定的胶束纳米药物。星形聚合物纳米药物表现出更好的治疗效果。由于胶束系统表现出略低的全身毒性,因此在给予等毒性剂量时,它们可能与星形可溶性系统具有相同的疗效。总之,研究中纳米药物的治疗效果直接受药物药代动力学的控制,即由于增强的通透性和保留(EPR)效应,它们能够在血液中循环足够长的时间,以有效积累在肿瘤中。易于规模化合成以及纳米药物应用的直接再制剂化可能性使这些纳米药物成为进一步临床评估的优秀候选者。

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