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ROS 响应介孔硅纳米颗粒用于磁共振成像引导的光动力操纵化疗。

ROS-responsive mesoporous silica nanoparticles for MR imaging-guided photodynamically maneuvered chemotherapy.

机构信息

School of Chemical Engineering, College of Engineering, Sungkyunkwan University, Suwon 16419, Republic of Korea.

出版信息

Nanoscale. 2018 May 24;10(20):9616-9627. doi: 10.1039/c8nr00888d.

DOI:10.1039/c8nr00888d
PMID:29756137
Abstract

Mesoporous silica nanoparticles (MSNs) with stimuli-responsive gatekeepers have been extensively investigated for controlled drug delivery at the target sites. Herein, we developed reactive oxygen species (ROS)-responsive MSNs (R-MSNs), consisting of a gadolinium (Gd)-DOTA complex as the ROS-responsive gatekeeper and polyethylene glycol (PEG)-conjugated chlorin e6 as the ROS generator, for magnetic resonance (MR) imaging-guided photodynamic chemotherapy. Doxorubicin (DOX), chosen as an anticancer drug, was physically encapsulated into DOTA-conjugated MSNs, followed by chemical crosslinking via the addition of GdCl3. DOX-R-MSNs could effectively maintain their structural integrity in a physiological environment for 7 days and show an enhanced in vitro T1-MR imaging signal for the Gd-DOTA complex. Upon 660 nm laser irradiation, the release rate of DOX from DOX-R-MSNs remarkably increased along with the disintegration of the gatekeeper, whereas DOX release was significantly retarded without irradiation. When DOX-R-MSNs were intravenously injected into tumor-bearing mice, they were effectively accumulated in tumor tissue, which was demonstrated using MR imaging. In addition, tumor growth was significantly suppressed by DOX-R-MSNs, allowing for site-specific release of DOX in a photodynamically maneuvered manner. Overall, these results suggest that R-MSNs have potential as drug carriers for MR imaging-guided photodynamic chemotherapy.

摘要

介孔硅纳米粒子(MSNs)具有刺激响应的门控剂,已被广泛研究用于在靶部位进行控制药物释放。在此,我们开发了活性氧(ROS)响应的 MSNs(R-MSNs),由钆(Gd)-DOTA 配合物作为 ROS 响应的门控剂和聚乙二醇(PEG)缀合的叶绿素 e6 作为 ROS 发生器,用于磁共振(MR)成像引导的光动力化疗。选择阿霉素(DOX)作为抗癌药物,通过添加 GdCl3 进行化学交联,将其物理包封在 DOTA 缀合的 MSNs 中。DOX-R-MSNs 在生理环境中能够有效保持其结构完整性 7 天,并表现出增强的体外 T1-MR 成像信号用于 Gd-DOTA 配合物。在 660nm 激光照射下,DOX 从 DOX-R-MSNs 的释放速率随着门控剂的崩解而显著增加,而没有照射时则显著延迟。当 DOX-R-MSNs 静脉注射到荷瘤小鼠体内时,它们能够有效聚集在肿瘤组织中,这可以通过磁共振成像来证明。此外,DOX-R-MSNs 显著抑制了肿瘤生长,允许以光动力方式在特定部位释放 DOX。总的来说,这些结果表明 R-MSNs 有潜力作为用于磁共振成像引导的光动力化疗的药物载体。

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