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用于光热/光动力协同治疗的具有肿瘤活性复合纳米系统的高穿透性和按需氧释放

Highly Penetrable and On-Demand Oxygen Release with Tumor Activity Composite Nanosystem for Photothermal/Photodynamic Synergetic Therapy.

作者信息

Wang Ya, Luo Siyuan, Wu Youshen, Tang Peng, Liu Jiajun, Liu Zeying, Shen Shihong, Ren Haozhe, Wu Daocheng

机构信息

Key Laboratory of Biomedical Information Engineering of the Ministry of Education, School of Life Science and Technology, Xi'an Jiaotong University, Xi'an 710049, P. R. China.

Department of Chemistry, School of Science, Xi'an Jiaotong University, Xi'an 710049, P. R. China.

出版信息

ACS Nano. 2020 Dec 22;14(12):17046-17062. doi: 10.1021/acsnano.0c06415. Epub 2020 Dec 8.

DOI:10.1021/acsnano.0c06415
PMID:33290657
Abstract

A deep penetrating and pH-responsive composite nanosystem was strategically developed to improve the efficacy of synergetic photothermal/photodynamic therapy (PTT/PDT) against hypoxic tumor. The designed nanosystem ([PHC]PP@HA NPs) was constructed by coloading hemoglobin (Hb) and chlorin e6 on polydopamine to build small-sized PHC NPs, which were encapsulated inside the polymer micelles (poly(ethylene glycol)-poly(ethylenimine)) and then capped with functionalized hyaluronic acid. The pH-responsive feature made [PHC]PP@HA NPs retain an initial size of ∼140 nm in blood circulation but rapidly release small PHC NPs (∼10 nm) with a high tumor-penetrating ability in the tumor microenvironment. The penetration experiment showed that the penetration depth of PHC NPs in the multicellular tumor spheroids exceeded 110 μm. The [PHC]PP@HA NPs exhibited excellent biocompatibility, deep tumor permeability, high photothermal conversion efficiency (47.09%), and low combination index (0.59) under hypoxic conditions. Notably, the nanosystem can freely adjust the release of oxygen and damaging PHC NPs in an on-demand manner on the basis of the feedback of tumor activity. This feedback tumor therapy significantly improved the synergistic effect of PTT/PDT and reduced its toxic side effects. The antitumor results showed that the tumor inhibition rate of [PHC]PP@HA NPs with an on-demand oxygen supply of Hb was ∼100%, which was much better than those of PTT alone and Hb-free nanoparticles ([PC]PP@HA NPs). Consequently, the [PHC]PP@HA NP-mediated PTT/PDT guided by feedback tumor therapy achieved an efficient tumor ablation with an extremely low tumor recurrence rate (8.3%) 60 d later, indicating the versatile potential of PTT/PDT.

摘要

为提高协同光热/光动力疗法(PTT/PDT)对缺氧肿瘤的疗效,精心研发了一种具有深层穿透能力和pH响应性的复合纳米系统。所设计的纳米系统([PHC]PP@HA NPs)通过将血红蛋白(Hb)和二氢卟吩e6共负载于聚多巴胺上构建小型PHC NPs,然后将其包裹在聚合物胶束(聚乙二醇-聚乙烯亚胺)中,再用功能化透明质酸进行封端。pH响应特性使[PHC]PP@HA NPs在血液循环中保持约140 nm的初始尺寸,但在肿瘤微环境中迅速释放出具有高肿瘤穿透能力的小型PHC NPs(约10 nm)。穿透实验表明,PHC NPs在多细胞肿瘤球体中的穿透深度超过110μm。[PHC]PP@HA NPs在缺氧条件下表现出优异的生物相容性、深层肿瘤渗透性、高光热转换效率(47.09%)和低联合指数(0.59)。值得注意的是,该纳米系统可根据肿瘤活性的反馈按需自由调节氧气和具有破坏作用的PHC NPs的释放。这种反馈式肿瘤治疗显著提高了PTT/PDT的协同效应并降低了其毒副作用。抗肿瘤结果显示,按需供应Hb的[PHC]PP@HA NPs的肿瘤抑制率约为100%,远优于单独的PTT和不含Hb的纳米颗粒([PC]PP@HA NPs)。因此,由反馈式肿瘤治疗引导的[PHC]PP@HA NP介导的PTT/PDT在60天后实现了高效的肿瘤消融,肿瘤复发率极低(8.3%),表明了PTT/PDT的多功能潜力。

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