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新型可生物降解的载甲氨蝶呤抗癌药物的分子印迹聚合物纳米粒的给药系统:合成、表征及细胞研究。

Novel biodegradable molecularly imprinted polymer nanoparticles for drug delivery of methotrexate anti-cancer; synthesis, characterization and cellular studies.

机构信息

Department of Drug and Food Control, Faculty of Pharmacy, Tehran University of Medical Sciences, Tehran, Iran.

Nanotechnology Research Center, Faculty of Pharmacy, Tehran University of Medical Sciences, Tehran, Iran.

出版信息

Daru. 2022 Dec;30(2):289-302. doi: 10.1007/s40199-022-00447-7. Epub 2022 Sep 10.

Abstract

BACKGROUND

Recently biodegradable nanoparticles are the center of attention for the development of drug delivery systems. Molecularly imprinted polymer (MIP) is an interesting candidate for designing drug nano-carriers. MIP-based nanoparticles could be used for cancer treatment and exhibited the potential to fill gaps regarding to ligand-based nanomaterials. Also, the presence of a cross-linker can play an essential role in nanoparticle stability and physicochemical properties of nanoparticles after synthesis.

OBJECTIVES

In this research, a biodegradable drug delivery system based on MIP nanoparticles was prepared using a biodegradable cross-linker (dimethacryloyl hydroxylamine, DMHA) for methotrexate (MTX). A hydrolysable functional group CO-O-NH-CO was added to the crosslinking agent to increase the final biodegradability of the polymer.

METHODS

Firstly, a biodegradable cross-linker was synthesized. Then, the non-imprinted polymers were prepared through mini-emulsion polymerization in the absence of a template; and efficient particle size distribution was determined. Finally, methotrexate was placed in imprinted polymers to achieve the desired MIP. Different types of MIPs were synthesized using different molar ratios of template, cross-linker, and functional monomer, and the optimal molar ratio was obtained at 1:4:20, respectively.

RESULTS

HNMR successfully confirmed the chemical structure of the cross-linker. According to SEM images, nanoparticles had a spherical shape with a smooth surface. The imprinted nanoparticles showed a narrow size distribution with an average of 120 nm at a high ratio of cross-linker. The drug loading and entrapment efficiency were 6.4% and 92%, respectively. The biodegradability studies indicated that the nanoparticles prepared by DMHA had a more degradability rate than ethylene glycol dimethacrylate as a conventional cross-linker. Also, the polymer degradation rate was higher in alkaline environments. Release studies in physiological and alkaline buffer showed an initial burst release of a quarter of loaded MTX during the day and a 70% release during a week. The Korsmeyer-Peppas model described the release pattern. The cytotoxicity of MTX loaded in nanoparticles was studied on the MCF-7 cell line, and the IC was 3.54 μg/ml.

CONCLUSION

It was demonstrated that nanoparticles prepared by DMHA have the potential to be used as biodegradable drug carriers for anticancer delivery. Synthesis schema of molecular imprinting of methotrexate in biodegradable polymer based on dimethacryloyl hydroxylamine cross-linker, for use as nanocarrier anticancer delivery to breast tumor.

摘要

背景

最近,可生物降解的纳米粒子是药物输送系统发展的焦点。分子印迹聚合物(MIP)是设计药物纳米载体的一个有趣的候选物。基于 MIP 的纳米粒子可用于癌症治疗,并显示出填补基于配体的纳米材料的空白的潜力。此外,交联剂的存在可以在纳米粒子的稳定性和合成后纳米粒子的物理化学性质中发挥重要作用。

目的

在这项研究中,使用可生物降解的交联剂(二甲基丙烯酰羟胺,DMHA)制备了基于 MIP 纳米粒子的可生物降解药物输送系统,用于甲氨蝶呤(MTX)。在交联剂中添加了可水解的 CO-O-NH-CO 官能团,以提高聚合物的最终生物降解性。

方法

首先,合成了一种可生物降解的交联剂。然后,通过无模板的小乳液聚合制备了非印迹聚合物,并确定了有效的粒径分布。最后,将甲氨蝶呤置于印迹聚合物中,以获得所需的 MIP。使用不同模板、交联剂和功能单体的摩尔比合成了不同类型的 MIP,并分别获得了最佳摩尔比为 1:4:20。

结果

HNMR 成功地证实了交联剂的化学结构。根据 SEM 图像,纳米粒子具有球形形状,表面光滑。印迹纳米粒子具有较窄的粒径分布,在高交联剂比下平均粒径为 120nm。药物负载和包封效率分别为 6.4%和 92%。生物降解研究表明,与传统交联剂乙二醇二甲基丙烯酸酯相比,由 DMHA 制备的纳米粒子具有更高的降解率。此外,聚合物在碱性环境中的降解速度更高。在生理和碱性缓冲液中的释放研究表明,在一天内有四分之一的负载 MTX 初始突释,在一周内有 70%的释放。Korsmeyer-Peppas 模型描述了释放模式。研究了载有 MTX 的纳米粒子对 MCF-7 细胞系的细胞毒性,IC 为 3.54μg/ml。

结论

结果表明,由 DMHA 制备的纳米粒子具有作为用于抗癌输送的可生物降解药物载体的潜力。基于二甲基丙烯酰羟胺交联剂的甲氨蝶呤分子印迹在可生物降解聚合物中的合成方案,用于制备作为抗癌递送的纳米载体用于乳腺癌。

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