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用于光热调制药物释放和协同光热治疗的热敏脂质体包裹金纳米笼

Thermosensitive liposome-encapsulated gold nanocages for photothermal-modulated drug release and synergistic photothermal therapy.

作者信息

Hao Ran, Jiao Meng, Xu Xingguo, Wu Di, Wei Haiying, Zeng Leyong

机构信息

College of Chemistry and Materials Science, Chemical Biology Key Laboratory of Hebei Province, Hebei Research Center of the Basic Discipline of Synthetic Chemistry, Hebei University, Baoding, 071002, P. R. China.

Department of Radiotherapy, Affiliated Hospital of Hebei University, Baoding 071000, P. R. China.

出版信息

J Mater Chem B. 2025 Feb 5;13(6):2042-2051. doi: 10.1039/d4tb02056a.


DOI:10.1039/d4tb02056a
PMID:39750526
Abstract

Delivery nanosystems have been widely developed to improve the efficacy of chemotherapy. However, their performance regarding the non-specific leakage of drugs remained unsatisfactory. Herein, gold nanocages (AuNCs) were used as carriers and thermo-sensitive liposome (TSL) as a protective shell to design a camptothecin (CPT)-loaded delivery nanosystem (AuNCs/CPT@TSL) for photothermal-modulated drug release. This approach effectively avoided the non-specific leakage of CPT and enabled the combination of photothermal therapy (PTT) and chemotherapy. In the simulated tumor microenvironment (pH = 5.5), the TSL shell prevented CPT leakage at 37 °C, with a release rate of only 11.4%. However, the release rate of CPT greatly increased to 85.4% when the temperature was elevated to 45 °C. The photothermal conversion efficiency of AuNCs/CPT@TSL reached up to 46.1%. At an incubation temperature of 37 °C, the cell survival rate decreased to 43.6% in AuNCs/CPT but remained above 90% in AuNCs/CPT@TSL, demonstrating the protective effect of the TSL shell. Under the combination of PTT and chemotherapy, cell viability drastically decreased to 10.9%, and the tumors completely disappeared, confirming the safe and reliable antitumor effect of AuNCs/CPT@TSL.

摘要

为提高化疗疗效,人们广泛开发了递送纳米系统。然而,其在药物非特异性渗漏方面的性能仍不尽人意。在此,金纳米笼(AuNCs)被用作载体,热敏脂质体(TSL)被用作保护壳,以设计一种负载喜树碱(CPT)的递送纳米系统(AuNCs/CPT@TSL)用于光热调制药物释放。这种方法有效避免了CPT的非特异性渗漏,并实现了光热疗法(PTT)和化疗的联合。在模拟肿瘤微环境(pH = 5.5)中,TSL壳在37℃时可防止CPT渗漏,释放率仅为11.4%。然而,当温度升高到45℃时,CPT的释放率大幅提高到85.4%。AuNCs/CPT@TSL的光热转换效率高达46.1%。在37℃的孵育温度下,AuNCs/CPT组的细胞存活率降至43.6%,而AuNCs/CPT@TSL组仍保持在90%以上,表明TSL壳具有保护作用。在PTT和化疗联合作用下,细胞活力急剧降至10.9%,肿瘤完全消失,证实了AuNCs/CPT@TSL安全可靠的抗肿瘤效果。

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[10]
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