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具有体内清除、ROS 清除和抗炎能力的多功能低温光热纳米药物。

Multifunctional low-temperature photothermal nanodrug with in vivo clearance, ROS-Scavenging and anti-inflammatory abilities.

机构信息

MOE Key Laboratory of Bioinorganic and Synthetic Chemistry, School of Chemistry, Sun Yat-Sen University, Guangzhou, 510275, PR China.

MOE Key Laboratory of Bioinorganic and Synthetic Chemistry, School of Chemistry, Sun Yat-Sen University, Guangzhou, 510275, PR China.

出版信息

Biomaterials. 2019 Sep;216:119280. doi: 10.1016/j.biomaterials.2019.119280. Epub 2019 Jun 14.

DOI:10.1016/j.biomaterials.2019.119280
PMID:31228705
Abstract

Harsh photothermal temperatures, long-term body retention of nanoagents, elevated ROS and inflammation induction all threaten the normal tissues, thus hindering the translation of photothermal therapy (PTT) from bench to clinical practice. To resolve these problems, we have developed a disassembled theranostic nanodrug Qu-FeP based on the quercetin coordination. Herein, quercetin is not only the heat shock protein (Hsp 70) inhibitor but also the skeleton of Qu-FeP, realizing near-infrared light induced low-temperature PTT (45 °C) to ablate tumor completely without heat stress to normal tissues. Owing to the ROS scavenging ability of quercetin, Qu-FeP effectively reduces intracellular ROS and in vivo inflammatory factors (TNF-α, IL-6, IFN-γ) levels. Simultaneously, quercetin-Fe coordination is weakened when scavenging ROS, which triggers the Qu-FeP disassembling, resulting in effective clearance of nanoparticles from main organs 168 h post intravenous injection. Additionally, the photoacoustic and magnetic resonance dual-imaging capability of Qu-FeP offers excellent spatial resolution and imaging depth not only for precise tumor diagnosis but also for monitoring the nanodrug disassembling in vivo. Thus, Qu-FeP intrinsically integrates precise diagnosis, excellent low-temperature PTT efficacy, ROS elimination and anti-inflammatory action, dynamic disassembly and renal clearance ability into a single nanodrug, which is very promising for future clinical cancer treatment.

摘要

苛刻的光热温度、纳米制剂在体内的长期滞留、活性氧(ROS)的升高和炎症的诱导都威胁着正常组织,从而阻碍了光热疗法(PTT)从实验室向临床实践的转化。为了解决这些问题,我们基于槲皮素的配位作用开发了一种可拆解的治疗性纳米药物 Qu-FeP。在此,槲皮素不仅是热休克蛋白(Hsp70)抑制剂,也是 Qu-FeP 的骨架,实现了近红外光诱导的低温 PTT(45°C),能够完全消融肿瘤,而不会对正常组织造成热应激。由于槲皮素的 ROS 清除能力,Qu-FeP 能够有效降低细胞内 ROS 和体内炎症因子(TNF-α、IL-6、IFN-γ)的水平。同时,当清除 ROS 时,槲皮素-Fe 配位被削弱,从而引发 Qu-FeP 的拆解,导致静脉注射后 168 小时内纳米颗粒从主要器官中有效清除。此外,Qu-FeP 的光声和磁共振双重成像能力不仅为精确的肿瘤诊断提供了优异的空间分辨率和成像深度,还能够监测体内纳米药物的拆解。因此,Qu-FeP 将精确诊断、优异的低温 PTT 疗效、ROS 消除和抗炎作用、动态拆解和肾脏清除能力内在地整合到单个纳米药物中,非常有希望应用于未来的临床癌症治疗。

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