Drug-Dependent Morphological Transitions in Spherical and Worm-Like Polymeric Micelles Define Stability and Pharmacological Performance of Micellar Drugs

Chaemin Lim, Jacob D. Ramsey, Duhyeong Hwang, S. Teixeira, C. Poon, J. Strauss, E. Rosen, M. Sokolsky-Papkov, A. Kabanov
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引用次数: 26

Abstract

Significant advances in physicochemical properties of polymeric micelles enable optimization of therapeutic drug efficacy, supporting nanomedicine manufacturing and clinical translation. Yet, the effect of micelle morphology on pharmacological efficacy has not been adequately addressed. We addressed this gap by assessing pharmacological efficacy of polymeric micelles with spherical and worm-like morphologies. We observed that poly(2-oxazoline)-based polymeric micelles can be elongated over time from a spherical structure to worm-like structure, with elongation influenced by several conditions, including the amount and type of drug loaded into the micelles. We further evaluated the role of different morphologies of olaparib micelles on pharmacological performance against a triple-negative breast cancer tumor (TNBC) model. Spherical micelles accumulated rapidly in the tumor tissue while retaining large amounts of drug; worm-like micelles accumulated more slowly and only upon releasing significant amounts of drug. These findings suggest that the dynamic character of the drug–micelle structure and the micelle morphology play a critical role in pharmacological performance, and that spherical micelles are better suited for systemic delivery of anticancer drugs to tumors when drugs are loosely associated with the polymeric micelles.
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球形和蠕虫状聚合物胶束的药物依赖形态转变决定了胶束药物的稳定性和药理性能
高分子胶束物理化学性质的重大进展使治疗药物疗效优化,支持纳米药物制造和临床转化。然而,胶束形态对药理学效果的影响尚未得到充分的解决。我们通过评估具有球形和蠕虫样形态的聚合物胶束的药理功效来解决这一差距。我们观察到,聚(2-恶唑啉)基聚合物胶束可以随着时间的推移从球形结构延伸到蠕虫状结构,其延伸率受到几个条件的影响,包括胶束中负载的药物的数量和类型。我们进一步评估了不同形态的奥拉帕尼胶束对三阴性乳腺癌(TNBC)模型的药理作用。球状胶束在肿瘤组织内迅速积聚,同时保留大量药物;蠕虫状胶束的积累速度更慢,只有在释放大量药物时才会积累。这些发现表明,药物胶束结构的动态特性和胶束形态对药物的药理性能起着至关重要的作用,当药物与聚合物胶束松散结合时,球形胶束更适合于将抗癌药物全身递送到肿瘤。
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Drug-Dependent Morphological Transitions in Spherical and Worm-Like Polymeric Micelles Define Stability and Pharmacological Performance of Micellar Drugs Nanopore Targeted Sequencing for the Accurate and Comprehensive Detection of SARS‐CoV‐2 and Other Respiratory Viruses
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