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制备具有提高的生物利用度和体外抗肿瘤功效的杨梅素负载的DSPE-PEG胶束。

Preparation of amentoflavone-loaded DSPE-PEG micelles with improved bioavailability and in vitro antitumor efficacy.

作者信息

Feng Yuan, Wang Jin, Zhang Shuaishuai, Li Yanan, Wang Boxin, Zhang Jiayuan, Qiu Yingzhe, Zhang Yi, Zhang Yuanyuan

机构信息

Hebei Key Laboratory of Neuropharmacology, Hebei North University, Zhangjiakou, China.

Shenyang Pharmaceutical University, Shenyang, China.

出版信息

Biomed Chromatogr. 2023 Sep;37(9):e5690. doi: 10.1002/bmc.5690. Epub 2023 Jun 19.

Abstract

To overcome the poor aqueous solubility and enhance the anticancer effects of amentoflavone (AF), a nontoxic and biodegradable amphiphilic copolymer, poly(ethyleneglycol)-distearoylphosphatidylethanolamine (DSPE-PEG ), was introduced to prepare AF micelles using the thin-film hydration method. Amentoflavone was successfully encapsulated into the core, achieving an encapsulation efficiency of 98.80 ± 0.24% and a drug loading efficiency of 2.96 ± 0.12%. The resulting micelles exhibited a spherical shape with a particle size of approximately 25.99 nm. The solubility of AF was significant improved by 412-fold, and cumulative drug release studies showed that AF release was much faster from the micelles compared with the free drug. The release of AF was sustained over time and followed a degradation-based kinetic model, similar to polymeric systems. After oral administration, the AF-loaded micelles demonstrated an enhanced oral bioavailability, which was 3.79 times higher than that of free AF. In vitro evaluations of the micelles' antitumor effects revealed a significantly greater efficacy compared with free AF. These findings highlight the tremendous potential of DSPE-PEG micelles as a drug delivery carrier for improving the solubility and therapeutic efficacy of AF.

摘要

为了克服穗花杉双黄酮(AF)水溶性差的问题并增强其抗癌效果,引入了一种无毒且可生物降解的两亲性共聚物聚乙二醇-二硬脂酰磷脂酰乙醇胺(DSPE-PEG),采用薄膜水化法制备AF胶束。穗花杉双黄酮成功包封于胶束核心,包封率达98.80±0.24%,载药率为2.96±0.12%。所得胶束呈球形,粒径约为25.99nm。AF的溶解度显著提高了412倍,累积药物释放研究表明,与游离药物相比,AF从胶束中的释放速度要快得多。AF的释放随时间持续进行,并遵循类似于聚合物体系的基于降解的动力学模型。口服给药后,载AF胶束的口服生物利用度提高,比游离AF高3.79倍。胶束抗肿瘤作用的体外评估显示,其疗效明显优于游离AF。这些发现突出了DSPE-PEG胶束作为药物递送载体在提高AF溶解度和治疗效果方面的巨大潜力。

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