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通过主体交换反应制备的包含碳硼烷的细胞外囊泡作为硼中子俘获治疗的硼载体。

Extracellular Vesicles Comprising Carborane Prepared by a Host Exchanging Reaction as a Boron Carrier for Boron Neutron Capture Therapy.

机构信息

Applied Chemistry Program, Graduate School of Advanced Science and Engineering, Hiroshima University, 1-4-1 Kagamiyama, Higashi-Hiroshima 739-8527, Japan.

Department of Applied Chemistry and Bioengineering, Graduate School of Engineering, Osaka Metropolitan University, 3-3-138 Sugimoto, Sumiyoshi-ku, Osaka 558-8585, Japan.

出版信息

ACS Appl Mater Interfaces. 2024 Sep 11;16(36):47137-47149. doi: 10.1021/acsami.4c07650. Epub 2024 Aug 6.

DOI:10.1021/acsami.4c07650
PMID:39106079
Abstract

With their low immunogenicity and excellent deliverability, extracellular vesicles (EVs) are promising platforms for drug delivery systems. In this study, hydrophobic molecule loading techniques were developed via an exchange reaction based on supramolecular chemistry without using organic solvents that can induce EV disruption and harmful side effects. To demonstrate the availability of an exchanging reaction to prepare drug-loading EVs, hydrophobic boron cluster carborane (CB) was introduced to EVs (CB@EVs), which is expected as a boron agent for boron neutron capture therapy (BNCT). The exchange reaction enabled the encapsulation of CB to EVs without disrupting their structure and forming aggregates. Single-particle analysis revealed that an exchanging reaction can uniformly introduce cargo molecules to EVs, which is advantageous in formulating pharmaceuticals. The performance of CB@EVs as boron agents for BNCT was demonstrated in vitro and in vivo. Compared to L-BPA, a clinically available boron agent, and CB delivered with liposomes, CB@EV systems exhibited the highest BNCT activity in vitro due to their excellent deliverability of cargo molecules via an endocytosis-independent pathway. The system can deeply penetrate 3D cultured spheroids even in the presence of extracellular matrices. The EV-based system could efficiently accumulate in tumor tissues in tumor xenograft model mice with high selectivity, mainly via the enhanced permeation and retention effect, and the deliverability of cargo molecules to tumor tissues in vivo enhanced the therapeutic benefits of BNCT compared to the L-BPA/fructose complex. All of the features of EVs are also advantageous in establishing anticancer agent delivery platforms.

摘要

由于细胞外囊泡 (EVs) 的免疫原性低、传递效率高,因此它们是药物传递系统的有前途的平台。在本研究中,开发了基于超分子化学的交换反应的疏水分子加载技术,而无需使用可能导致 EV 破坏和有害副作用的有机溶剂。为了证明交换反应可用于制备载药 EVs,将疏水分子硼簇碳硼烷 (CB) 引入 EVs(CB@EVs)中,预计其将作为硼中子俘获治疗 (BNCT) 的硼试剂。交换反应使 CB 能够包封到 EVs 中,而不会破坏其结构并形成聚集体。单颗粒分析表明,交换反应可以均匀地将货物分子引入 EVs,这有利于药物制剂的形成。CB@EVs 作为 BNCT 的硼试剂的性能在体外和体内得到了证明。与临床可用的硼试剂 L-BPA 和用脂质体递送的 CB 相比,由于其通过非内吞途径传递货物分子的优异传递效率,CB@EV 系统在体外表现出最高的 BNCT 活性。该系统即使在存在细胞外基质的情况下,也可以深入穿透 3D 培养的球体。基于 EV 的系统在肿瘤异种移植模型小鼠中具有高度选择性,能够有效地在肿瘤组织中积累,主要是通过增强的渗透和保留效应,并且货物分子向肿瘤组织的传递效率提高了 BNCT 的治疗效果,优于 L-BPA/果糖复合物。EVs 的所有特征也有利于建立抗癌药物传递平台。

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引用本文的文献

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