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双 miRNA 触发的药物释放系统用于逻辑运算的联合化疗和基因治疗

Dual MicroRNA-Triggered Drug Release System for Combined Chemotherapy and Gene Therapy with Logic Operation.

机构信息

The Key Lab of Health Chemistry and Molecular Diagnosis of Suzhou College of Chemistry, Chemical Engineering and Materials Science, Soochow University, 199 Ren'ai Road, Suzhou 215123, P. R. China.

出版信息

ACS Appl Mater Interfaces. 2020 Jul 22;12(29):32493-32502. doi: 10.1021/acsami.0c09494. Epub 2020 Jul 7.

DOI:10.1021/acsami.0c09494
PMID:32573191
Abstract

Combination therapy via stimulus-responsive drug release is known to improve treatment efficacy and minimize side effects. However, the use of low-abundance cancer biomarkers as molecular triggers to induce efficient drug release for combination therapy still remains a challenge. Herein, we developed a dual microRNA-responsive drug nanocarrier for catalytic release of doxorubicin (Dox) and small interfering RNA (siRNA) in cancerous cells for combined chemotherapy and gene therapy with logic operation. The nanocarrier is constructed by assembling two duplexes of DNA/RNA and Dox molecules onto DNA-functionalized gold nanoparticles. Two microRNA molecules (miRNA-21 and miRNA-10b overexpressed in MDA-MB-231) could alternatively catalyze the disassembly of the nanocarrier through a thermodynamically driven entropy gain process, during which Dox molecules are released, and the two pairs of released DNA/RNA duplex hybridize to generate siRNA (siBcl-2) in situ by strand displacement reactions. Quantum dots are used to track the process in living cells. The AND logic gate-based drug release system allows effective treatment of specific cancer cell types according to miRNA expression patterns. This strategy represents an effective means to overcome multidrug resistance and improve therapeutic effects.

摘要

联合治疗通过刺激响应药物释放被认为可以提高治疗效果并最小化副作用。然而,使用低丰度的癌症生物标志物作为分子触发物来诱导有效的药物释放以进行联合治疗仍然是一个挑战。在这里,我们开发了一种双 microRNA 响应性药物纳米载体,用于在癌细胞中催化释放阿霉素 (Dox) 和小干扰 RNA (siRNA),用于具有逻辑操作的联合化疗和基因治疗。该纳米载体通过将两个双链 DNA/RNA 和 Dox 分子组装到 DNA 功能化的金纳米粒子上来构建。两种 microRNA 分子(miRNA-21 和 miRNA-10b 在 MDA-MB-231 中过表达)可以通过热力学驱动的熵增过程交替催化纳米载体的解组装,在此过程中释放 Dox 分子,并且两对释放的 DNA/RNA 双链通过链置换反应就地杂交生成 siRNA (siBcl-2)。量子点用于在活细胞中跟踪该过程。基于 AND 逻辑门的药物释放系统允许根据 microRNA 表达模式对特定的癌细胞类型进行有效治疗。这种策略代表了克服多药耐药性和提高治疗效果的有效手段。

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