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光响应型空心二氧化硅纳米颗粒用于光触发基因和光动力协同治疗。

Photo-responsive hollow silica nanoparticles for light-triggered genetic and photodynamic synergistic therapy.

机构信息

The United Innovation of Mengchao Hepatobiliary Technology Key Laboratory of Fujian Province, Mengchao Hepatobiliary Hospital of Fujian Medical University, Fuzhou 350025, PR China; The Liver Center of Fujian Province, Fujian Medical University, Fuzhou 350025, PR China.

School of Basic Medical Sciences, Fujian Medical University, Fuzhou 350122, PR China.

出版信息

Acta Biomater. 2018 Aug;76:178-192. doi: 10.1016/j.actbio.2018.07.007. Epub 2018 Jul 4.

Abstract

UNLABELLED

The development of multifunctional carriers incorporating genetic and photodynamic therapy (PDT) for synergistic antitumor treatment has attracted intensive interests very recently. However, most of the currently reported systems employ passive gene release strategies depending on tumor microenvironment, which are negatively affected by the heterogeneity of cancer cells, thus resulting in limited controllability in therapeutic progress. Herein, a novel photo-responsive hollow silica nanoparticle (HNP)-based gene and photosensitizer (PS) co-delivery nanovehicle is designed for dual-wavelength light-triggered synergistic gene and PDT therapy. The resultant HNP conjugated with PDMAEMA polycation through a 405-nm light-cleavable Cou-linker, namely, HNP-Cou-PD, exhibits excellent gene condensation capacity, good biocompatibility, outstanding PS loading ability, and light-triggered gene release properties. HNP-Cou-PD with Chlorin e6 (Ce6) loaded inside the silica cavity and a plasmid encoding caspase-8 gene (CSP8) attached to the PDMAEMA outside layer (Ce6-HNP-Cou-PD/CSP8) has been proven to possess better antitumor effects under the irradiation of pre-405-nm and post-670-nm light both in vitro and in vivo because of the light-triggered intracellular gene release and reactive oxygen species (ROS) generation. Therefore, HNP-Cou-PD designed as a gene and PS co-delivery carrier might have promising applications in the future to precisely treat various types of cancers.

STATEMENT OF SIGNIFICANCE

Multifunctional carriers incorporating genetic and photodynamic therapy (PDT) have drawn intense attention very recently, ascribing to their enhanced anticancer effects. However, in the present gene and PDT synergistic system, gene release strategies passively relying on tumor microenvironment often result in no or poor controllability compared with PDT (a spatial and temporal therapeutic modal), which may hinder their synergistic efficacy, especially in an on-demand manner. To resolve this problem, we designed a hollow silica nanoparticle-based dual-wavelength light-responsive gene and photosensitizer (PS) co-delivery platform to achieve photo-triggered gene and PDT synergistic therapy. We believe that our work may have extensive application prospects in precise treatment of various cancers and be of interest to the readership.

摘要

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最近,将遗传和光动力疗法(PDT)相结合的多功能载体的发展引起了人们的浓厚兴趣。然而,目前大多数报道的系统采用依赖肿瘤微环境的被动基因释放策略,这受到癌细胞异质性的负面影响,因此在治疗进展方面的可控性有限。在此,设计了一种新型光响应的空心二氧化硅纳米粒子(HNP)基基因和光敏剂(PS)共递药纳米载体,用于双波长光触发协同基因和 PDT 治疗。所得的通过 405nm 光可裂解 Cou-linker 与 PDMAEMA 聚阳离子偶联的 HNP,即 HNP-Cou-PD,表现出优异的基因凝聚能力、良好的生物相容性、优异的 PS 负载能力和光触发基因释放特性。负载在二氧化硅腔内的氯 e6(Ce6)和附着在 PDMAEMA 外层的编码 Caspase-8 基因(CSP8)的 HNP-Cou-PD(Ce6-HNP-Cou-PD/CSP8)已被证明在体外和体内都具有更好的抗肿瘤效果,因为它在 405nm 前光和 670nm 后光的照射下具有光触发的细胞内基因释放和活性氧(ROS)生成。因此,作为基因和 PS 共递药载体的 HNP-Cou-PD 可能在未来具有精确治疗各种类型癌症的应用前景。

意义声明

将遗传和光动力疗法(PDT)相结合的多功能载体最近引起了人们的极大关注,这归因于它们增强的抗癌效果。然而,在目前的基因和 PDT 协同系统中,被动依赖肿瘤微环境的基因释放策略与 PDT(一种时空治疗模式)相比,往往无法实现或控制不佳,这可能会阻碍它们的协同疗效,尤其是在按需方式下。为了解决这个问题,我们设计了一种基于空心二氧化硅纳米粒子的双波长光响应基因和光敏剂(PS)共递药平台,以实现光触发基因和 PDT 协同治疗。我们相信,我们的工作可能在精确治疗各种癌症方面具有广泛的应用前景,并且对读者有兴趣。

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