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热敏病毒样颗粒用于癌症药物的靶向递送。

Thermally-responsive Virus-like Particle for Targeted Delivery of Cancer Drug.

机构信息

Department of Microbiology, Faculty of Biotechnology and Biomolecular Sciences, Universiti Putra Malaysia, 43400 UPM, Serdang, Selangor, Malaysia.

Department of Microbiology, College of Science, Agriculture and Modern Technologies, Shiraz Branch, Islamic Azad University, Shiraz, Iran.

出版信息

Sci Rep. 2019 Mar 8;9(1):3945. doi: 10.1038/s41598-019-40388-x.

Abstract

Multifunctional nanocarriers displaying specific ligands and simultaneously response to stimuli offer great potentials for targeted and controlled drug delivery. Several synthetic thermally-responsive nanocarriers have been studied extensively for hyperthermia incorporated chemotherapy. However, no information is available on the application of virus-like particle (VLP) in thermally-controlled drug delivery systems. Here, we describe the development of a novel multifunctional nanovehicle based on the VLP of Macrobrachium rosenbergii nodavirus (MrNVLP). Folic acid (FA) was covalently conjugated to lysine residues located on the surface of MrNVLP, while doxorubicin (Dox) was loaded inside the VLP using an infusion method. This thermally-responsive nanovehicle, namely FA-MrNVLP-Dox, released Dox in a sustained manner and the rate of drug release increased in response to a hyperthermia temperature at 43 °C. The FA-MrNVLP-Dox enhanced the delivery of Dox to HT29 cancer cells expressing high level of folate receptor (FR) as compared to CCD841CoN normal cells and HepG2 cancer cells, which express low levels of FR. As a result, FA-MrNVLP-Dox increased the cytotoxicity of Dox on HT29 cells, and decreased the drug's cytotoxicity on CCD841CoN and HepG2 cells. This study demonstrated the potential of FA-MrNVLP-Dox as a thermally-responsive nanovehicle for targeted delivery of Dox to cancer cells rich in FR.

摘要

多功能纳米载体展示特定的配体并同时响应刺激,为靶向和控制药物输送提供了巨大的潜力。已经广泛研究了几种合成的热响应纳米载体用于联合化疗的热疗。然而,关于病毒样颗粒 (VLP) 在热控药物传递系统中的应用尚无信息。在这里,我们描述了基于罗氏沼虾诺达病毒 (MrNVLP) 的 VLP 的新型多功能纳米载体的开发。叶酸 (FA) 通过共价键连接到 MrNVLP 表面的赖氨酸残基上,而阿霉素 (Dox) 则通过灌注法加载到 VLP 内部。这种热响应纳米载体,即 FA-MrNVLP-Dox,以持续的方式释放 Dox,并且药物释放率随着 43°C 的热疗温度的升高而增加。与表达低水平 FR 的 CCD841CoN 正常细胞和 HepG2 癌细胞相比,FA-MrNVLP-Dox 增强了 Dox 向表达高水平 FR 的 HT29 癌细胞的递送。结果,FA-MrNVLP-Dox 增加了 Dox 对 HT29 细胞的细胞毒性,降低了 Dox 对 CCD841CoN 和 HepG2 细胞的细胞毒性。这项研究表明,FA-MrNVLP-Dox 作为一种热响应纳米载体,具有将 Dox 靶向递送至富含 FR 的癌细胞的潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f94b/6408444/a3b96df1e66f/41598_2019_40388_Fig1_HTML.jpg

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