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Physico-Chemical Strategies to Enhance Stability and Drug Retention of Polymeric Micelles for Tumor-Targeted Drug Delivery

机译:物理化学策略,以增强针对肿瘤靶向药物输送的聚合物胶束的稳定性和药物保留能力。

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摘要

Polymeric micelles (PM) have been extensively used for tumor-targeted delivery of hydrophobic anti-cancer drugs. The lipophilic core of PM is naturally suitable for loading hydrophobic drugs and the hydrophilic shell endows them with colloidal stability and stealth properties. Decades of research on PM have resulted in tremendous numbers of PM-forming amphiphilic polymers, and approximately a dozen micellar nanomedicines have entered the clinic. The first generation of PM can be considered solubilizers of hydrophobic drugs, with short circulation times resulting from poor micelle stability and unstable drug entrapment. To more optimally exploit the potential of PM for targeted drug delivery, several physical (e.g., π–π stacking, stereocomplexation, hydrogen bonding, host–guest complexation, and coordination interaction) and chemical (e.g., free radical polymerization, click chemistry, disulfide and hydrazone bonding) strategies have been developed to improve micelle stability and drug retention. In this review, the most promising physico-chemical approaches to enhance micelle stability and drug retention are described, and how these strategies have resulted in systems with promising therapeutic efficacy in animal models, paving the way for clinical translation, is summarized.
机译:聚合物胶束(PM)已被广泛用于疏水性抗癌药物的肿瘤靶向递送。 PM的亲脂性核心天然适合装载疏水性药物,亲水性外壳赋予它们胶体稳定性和隐身性。数十年来对PM的研究已导致形成大量PM的两亲性聚合物,并且大约有十二种胶束纳米药物已进入临床。第一代PM可以认为是疏水性药物的增溶剂,由于胶束稳定性差和药物截留不稳定,循环时间短。为了更充分地利用PM进行靶向药物输送的潜力,可以使用几种物理方法(例如,π-π堆积,立体复合,氢键,主体-客体复合和配位相互作用)和化学方法(例如,自由基聚合,点击化学,二硫化物)和键)策略已被开发来改善胶束稳定性和药物保留。在这篇综述中,描述了增强胶束稳定性和药物保留的最有前途的物理化学方法,并总结了这些策略如何在动物模型中产生具有良好治疗效果的系统,为临床翻译铺平了道路。

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