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探究多孔配位笼用于增强癌症纳米治疗的亚细胞区室靶向效应。

Investigating Subcellular Compartment Targeting Effect of Porous Coordination Cages for Enhancing Cancer Nanotherapy.

机构信息

Department of Chemistry, Texas A&M University, College Station, TX, 77843, USA.

Beijing National Laboratory for Molecular Sciences, CAS Key Laboratory of Analytical Chemistry for Living Biosystems, Institute of Chemistry, Chinese Academy of Sciences, Beijing, 100190, China.

出版信息

Small. 2018 Nov;14(47):e1802709. doi: 10.1002/smll.201802709. Epub 2018 Sep 17.

Abstract

Understanding the key factors for successful subcellular compartment targeting for cargo delivery systems is of great interest in a variety of fields such as bionanotechnology, cell biology, and nanotherapies. However, the fundamental basis for intracellular transportation with these systems has thus far rarely been discussed. As a cargo vector, porous coordination cages (PCCs) have great potential for use in cancer nanotherapy and to elucidate fundamental insight regarding subcellular compartment targeting. Herein, it is shown that the transportation of PCC cargo vectors though various subcellular barriers of the mammalian cell can be manipulated by tuning the vector's electronic property and surface affinity. It is found that the PCCs become selectively aggregated at the cell membrane, the cytoplasm, or the nucleus, respectively. When a DNA topoisomerase inhibitor is delivered into the nucleus by a neutral and lipophilic PCC, the anticancer efficacy is dramatically improved. The findings shed light to tune the interactions at the "bio-nano" interface. This study provides a key strategy for future work in targeting specific cell organelles for cell imaging, cargo delivery, and therapy. This research also offers key insight into the engineering of nanoscopic materials for furnishing cell organelle-specificity.

摘要

了解货物输送系统亚细胞区室靶向成功的关键因素在生物纳米技术、细胞生物学和纳米疗法等多个领域都具有重要意义。然而,迄今为止,对于这些系统的细胞内运输的基本原理还很少被讨论。作为货物载体,多孔配位笼(PCCs)在癌症纳米治疗中有很大的应用潜力,并能阐明亚细胞区室靶向的基本见解。本文表明,可以通过调节载体的电子性质和表面亲和力来操纵 PCC 货物载体通过哺乳动物细胞的各种亚细胞屏障的运输。研究发现,PCC 分别在细胞膜、细胞质或细胞核处选择性聚集。当一种 DNA 拓扑异构酶抑制剂被一种中性和亲脂性的 PCC 递送到细胞核中时,其抗癌效果显著提高。这些发现为在“生物-纳米”界面上调节相互作用提供了依据。本研究为针对特定细胞细胞器进行细胞成像、货物输送和治疗的靶向特定细胞细胞器提供了关键策略。该研究还为用于提供细胞器特异性的纳米级材料的工程提供了关键的见解。

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