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载有美金刚的聚乙二醇化单壁碳纳米管分散体的配方与优化

Formulation and Optimization of Memantine-Loaded PEGylated Single-Walled Carbon Nanotube Dispersions.

作者信息

Le Hoa, Nguyen Hai V, Abioye Amos, Adejare Adeboye

机构信息

Department of Pharmaceutical Sciences, Philadelphia College of Pharmacy (PCP), Saint Joseph's University, Philadelphia, PA, USA.

Department of Pharmaceutical Industry, Hanoi University of Pharmacy, Hanoi, Vietnam.

出版信息

AAPS PharmSciTech. 2025 Sep 19;26(8):231. doi: 10.1208/s12249-025-03194-5.

Abstract

The study aimed to develop stable single-walled carbon nanotube (SWCNT) dispersions in water that exhibit low protein adsorption in biological media, entrap Memantine, and release the drug in a controlled manner. Specifically, SWCNTs were functionalized, initially oxidized, and then non-covalently conjugated with pyrene methoxy polyethylene glycols (PEG). Dynamic light scattering, Raman spectroscopy, and Fourier-transform infrared spectroscopy were used to evaluate various physicochemical properties of PEG functionalized SWCNTs (PEGSWCNTs). A D-optimal design, utilizing JMP Pro 16, was employed to design the experiment and investigate the effects of oxidation time and PEG concentration on the physicochemical properties of SWCNT dispersions. The optimal dispersions exhibited hydrodynamic particle sizes, polydispersity indices, and zeta potentials ranging from 157.5 to 204.4 nm, 0.231 to 0.255, and -27.8 to -18.8 mV, respectively. The interaction between serum proteins and PEGSWCNTs was evaluated using dynamic light scattering, bicinchoninic acid, and sodium dodecyl sulfate-polyacrylamide gel electrophoresis. The serum protein-SWCNT interaction was significantly reduced due to the presence of PEGs, depending on PEG concentrations, the ratio of long-chain PEG molecules to short-chain PEG molecules, and the physicochemical properties of PEGSWCNT dispersions. Finally, Memantine was incorporated into the optimal PEGSWCNT dispersions. The entrapment efficiency, drug loading, and drug release from the dispersions were evaluated using gas chromatography with flame ionization detection (GC/FID). The results indicated that PEGSWCNT particles could entrap Memantine. The in vitro drug release profile exhibited an extended release over 3 to 7 h, with a significant burst release occurring in the first hour (more than 50%). Higher PEG density and a higher PEG20K/2K ratio exhibited slower drug release rates. The release profiles of the formulations using 40% PEG were fitted to the Weibull model, indicating that Memantine release from the SWCNT dispersions followed a Fickian diffusion mechanism.

摘要

该研究旨在开发在水中稳定的单壁碳纳米管(SWCNT)分散体,其在生物介质中表现出低蛋白吸附性,能包载美金刚,并以可控方式释放药物。具体而言,对SWCNT进行功能化处理,先氧化,然后与芘甲氧基聚乙二醇(PEG)进行非共价共轭。使用动态光散射、拉曼光谱和傅里叶变换红外光谱来评估PEG功能化SWCNT(PEGSWCNT)的各种物理化学性质。利用JMP Pro 16采用D最优设计来设计实验,并研究氧化时间和PEG浓度对SWCNT分散体物理化学性质的影响。最佳分散体的流体动力学粒径、多分散指数和zeta电位分别为157.5至204.4 nm、0.231至0.255和-27.8至-18.8 mV。使用动态光散射、二辛可宁酸和十二烷基硫酸钠-聚丙烯酰胺凝胶电泳评估血清蛋白与PEGSWCNT之间的相互作用。由于PEG的存在,血清蛋白与SWCNT的相互作用显著降低,这取决于PEG浓度、长链PEG分子与短链PEG分子的比例以及PEGSWCNT分散体的物理化学性质。最后,将美金刚掺入最佳的PEGSWCNT分散体中。使用带有火焰离子化检测的气相色谱法(GC/FID)评估分散体的包封率、载药量和药物释放情况。结果表明,PEGSWCNT颗粒能够包载美金刚。体外药物释放曲线显示在3至7小时内呈现缓释,在第一小时出现显著的突释(超过50%)。较高的PEG密度和较高的PEG20K/2K比例表现出较慢的药物释放速率。使用40% PEG的制剂的释放曲线符合威布尔模型,表明美金刚从SWCNT分散体中的释放遵循菲克扩散机制。

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