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用于克服多药耐药肿瘤的金纳米星的近红外光可裂解药物加合物。

NIR-cleavable drug adducts of gold nanostars for overcoming multidrug-resistant tumors.

机构信息

Department of Biomedical Engineering and Environmental Sciences, National Tsing Hua University, Hsinchu, 30013 Taiwan, Republic of China.

Department of Bioscience and Biotechnology, National Taiwan Ocean University, Keelung, 20224, Taiwan, Republic of China.

出版信息

Biomater Sci. 2020 Mar 31;8(7):1934-1950. doi: 10.1039/c9bm01813a.

Abstract

An aptamer-conjugated gold nanostar (dsDDA-AuNS) has been developed for targeting nucleolin present in both tumor cells and tumor vasculature for conducting a drug-resistant cancer therapy. AuNS with its strong absorption in the near-infrared (NIR) region was assembled with a layer of the anti-nucleolin aptamer AS1411. An anticancer drug, namely doxorubicin (DOX), was specifically conjugated on deoxyguanosine residues employing heat and acid labile methylene linkages. In response to NIR irradiation, dsDDA-AuNS allowed on-demand therapeutics. AS1411 played an active role in drug cargo-nucleus interactions, enhancing drug accumulation in the nuclei of drug-resistant breast cancer cells. The intravenous injection of dsDDA-AuNS allowed higher drug accumulation in drug-resistant tumors over naked drugs, leading to greater therapeutic efficacy even at a 54-fold less equivalent drug dose. The in vivo triggered release of DOX from dsDDA-AuNS was achieved by NIR irradiation, resulting in simultaneous photothermal and chemotherapeutic actions, yielding superior tumor growth inhibition than those obtained from either type of monotherapy for overcoming drug resistance in cancers.

摘要

一种适配体偶联的金纳米星(dsDDA-AuNS)已被开发用于靶向肿瘤细胞和肿瘤血管中的核仁素,以进行耐药性癌症治疗。具有近红外(NIR)区域强吸收的 AuNS 与一层抗核仁素适配体 AS1411 组装在一起。一种抗癌药物,即阿霉素(DOX),通过热和酸不稳定的亚甲基键特异性地连接在脱氧鸟苷残基上。响应 NIR 照射,dsDDA-AuNS 允许按需治疗。AS1411 在药物货物-核相互作用中发挥积极作用,增强了耐药乳腺癌细胞中药物在核内的积累。与裸药相比,dsDDA-AuNS 的静脉注射允许在耐药肿瘤中积累更高的药物,即使在 54 倍低等效药物剂量下,也能获得更好的治疗效果。通过 NIR 照射从 dsDDA-AuNS 中实现 DOX 的体内触发释放,导致光热和化学治疗联合作用,比单一治疗获得的肿瘤生长抑制更好,从而克服癌症中的耐药性。

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