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可控组装/拆卸多酚-DNA 纳米复合物,用于癌细胞中级联响应药物释放。

Controllable assembly/disassembly of polyphenol-DNA nanocomplex for cascade-responsive drug release in cancer cells.

机构信息

Frontiers Science Center for Synthetic Biology, Key Laboratory of Systems Bioengineering (MOE), School of Chemical Engineering and Technology, Tianjin University, Tianjin, 300350, PR China.

School of Chemical Engineering and Australian Centre for NanoMedicine, University of New South Wales, Sydney, NSW, 2052, Australia.

出版信息

Biomaterials. 2021 Jun;273:120846. doi: 10.1016/j.biomaterials.2021.120846. Epub 2021 Apr 23.

Abstract

Developing nanocarrier systems with sufficient drug loading ability and efficient drug release behavior in cells is a powerful strategy to maximize therapeutic efficacies and minimize side effects of administered drugs. However, the two aspects are usually contradictory in a single nanocarrier. Herein, polyphenol-DNA nanocomplex with controllable assembly/disassembly behaviors is developed for responsive and sequential drug release in cancer cells. Programmable assembly of branched-DNA achieves multiple-gene loading, afterwards tannic acid (TA), plant-derived polyphenols as drugs mediate assembly of branched-DNA to form nanocomplex. Intracellularly, two-step disassembly process of nanocomplex enables efficient gene/drug release. Lysosomal acidic microenvironment induces the disassembly of nanocomplex to release TA and branched-DNA. Glutathione and DNase I in cytoplasm trigger the precise release of genes from branched-DNA. The efficacy of multiple-gene/chemo-therapy is demonstrated using in vitro and in vivo models. This work provides a controllable assembly/disassembly route to resolve the conflict between sufficient drug loading and efficient drug release in cells for therapeutics.

摘要

开发具有足够药物载药能力和高效细胞内药物释放行为的纳米载体系统是最大限度提高治疗效果和最小化给药药物副作用的有效策略。然而,在单个纳米载体中,这两个方面通常是矛盾的。本文中,设计了具有可控组装/解组装行为的多酚-DNA 纳米复合物,用于在癌细胞中进行响应性和顺序药物释放。支化 DNA 的可编程组装实现了多基因加载,然后单宁酸(TA),植物来源的多酚类药物介导支化 DNA 的组装以形成纳米复合物。在细胞内,纳米复合物的两步解组装过程实现了高效的基因/药物释放。溶酶体酸性微环境诱导纳米复合物的解组装以释放 TA 和支化 DNA。细胞质中的谷胱甘肽和 DNase I 触发基因从支化 DNA 的精确释放。体外和体内模型证明了多基因/化疗的疗效。这项工作为解决细胞内充分药物载药和高效药物释放之间的冲突提供了一种可控的组装/解组装途径,用于治疗。

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