两亲嵌段共聚物的纳米级自组装作为药物输送的有效模板

Dhruvi Patel, K. Kuperkar, S. Yusa, P. Bahadur
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摘要

这篇综述文章强调了目前在水溶液中各种嵌段共聚物(BCPs)自组装所形成的各种纳米结构聚合体的形成和特性方面所取得的进展。我们研究了不同聚合技术的发展情况,这些技术可以生产出具有所需预定分子量和低分散性的聚合物,并将其应用于技术和生物医学领域,特别是作为药物输送系统的载体。讨论了两亲性 BCP 和双亲水嵌段共聚物(DHBC)的溶液行为,其中一个或两个嵌段对任何刺激都有反应。此外,还详细介绍了聚电解质中性的 BCP 与带对立电荷的物质通过静电作用产生的聚离子复合胶束(PICM)/聚合体。最后,还揭示了聚合诱导自组装(PISA),它可形成尺寸/形状/表面功能可控的纳米级胶束聚集体,以及当 BCP 的一个嵌段可结晶时,可促进半结晶 BCP 的结晶驱动自组装。报告强调了共聚胶束在目前用于临床试验、研究或临床前测试的给药系统和药物制剂中的可扩展性,因为这些胶束将来可用于制造新型纳米药物。研究还考虑了最新文献和 BCP 自组装的未来前景。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Nanoscale Self-Assemblies from Amphiphilic Block Copolymers as Proficient Templates in Drug Delivery
This review article emphasizes the current enlargements in the formation and properties of the various nanostructured aggregates resulting from the self-assembly of a variety of block copolymers (BCPs) in an aqueous solution. The development of the different polymerization techniques which produce polymers with a desired predetermined molecular weight and low polydispersity is investigated with regard to their technological and biomedical applications; in particular, their applications as vehicles for drug delivery systems are considered. The solution behavior of amphiphilic BCPs and double-hydrophilic block copolymers (DHBCs), with one or both blocks being responsive to any stimulus, is discussed. Polyion complex micelles (PICMs)/polymersomes obtained from the electrostatic interaction of a polyelectrolyte-neutral BCP with oppositely charged species are also detailed. Lastly, polymerization-induced self-assembly (PISA), which forms nanoscale micellar aggregates with controlled size/shape/surface functionality, and the crystallization-driven self-assembly of semicrystalline BCPs facilitated when one block of the BCP is crystallizable, are also revealed. The scalability of the copolymeric micelles in the drug delivery systems and pharmaceutical formations that are currently being used in clinical trials, research, or preclinical testing is emphasized as these micelles could be used in the future to create novel nanomedicines. The updated literature and the future perspectives of BCP self-assembly are considered.
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