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基于超分子环糊精的药物纳米载体

Supramolecular cyclodextrin-based drug nanocarriers.

作者信息

Simões Susana M N, Rey-Rico Ana, Concheiro Angel, Alvarez-Lorenzo Carmen

机构信息

Faculty of Pharmacy, University of Coimbra, Coimbra, Portugal.

出版信息

Chem Commun (Camb). 2015 Apr 14;51(29):6275-89. doi: 10.1039/c4cc10388b.


DOI:10.1039/c4cc10388b
PMID:25679097
Abstract

Supramolecular systems formed by the binding of several cyclodextrins (CDs) to polymers or lipids, either via non-covalent or covalent links, open a wide range of possibilities for the delivery of active substances. CDs can perform as multifunctionalizable cores to which very diverse (macro)molecules and drugs can be conjugated. Grafting with amphiphilic molecules can lead to nanoassemblies exhibiting a variety of architectures. CDs can also polymerize with other CDs or can be used to functionalize preexisting polymers to form polymers/networks with enhanced capability to form inclusion complexes. Alternatively, CDs can be exploited as transient cross-linkers to form poly(pseudo)rotaxane-based networks or zipper-like assemblies. Combination of mutifunctionality and complexation ability of CDs has been shown to be useful to develop depot-like formulations and colloidal nanocarriers with improved performances regarding easiness of administration, protection of the encapsulated substances, control of the delivery rate, and cell interactions. The aim of this review is to provide an overall view of the diversity of designs of CD-based supramolecular nanosystems with a special focus on the advances materialized in the last five years, including clinical trials.

摘要

由几种环糊精(CDs)通过非共价或共价连接与聚合物或脂质结合形成的超分子体系,为活性物质的递送开辟了广泛的可能性。环糊精可以作为多功能化的核心,多种(大)分子和药物可以与之共轭。用两亲分子接枝可导致呈现各种结构的纳米组装体。环糊精还可以与其他环糊精聚合,或者用于使预先存在的聚合物功能化,以形成具有增强的形成包合物能力的聚合物/网络。或者,环糊精可以用作瞬态交联剂,以形成基于聚(假)轮烷的网络或拉链状组装体。环糊精的多功能性和络合能力的结合已被证明有助于开发具有改进性能的长效制剂和胶体纳米载体,这些性能包括给药便利性、对包封物质的保护、释放速率的控制以及细胞相互作用。本综述的目的是全面介绍基于环糊精的超分子纳米系统的设计多样性,特别关注过去五年中取得的进展,包括临床试验。

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