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海藻酸钠/N-(乙烯基己内酰胺)基于超分子自组装皮下给药原位形成的 5-氟尿嘧啶储存库:流变学分析、体外细胞毒性潜力、体内生物利用度和安全性评价。

Sodium alginate/N-(Vinylcaprolactam) based supramolecular self-assembled subcutaneously administered in situ formed gels depot of 5-fluorouracil: Rheological analysis, in vitro cytotoxic potential, in vivo bioavailability and safety evaluation.

机构信息

Margalla College of Pharmacy, Margalla Institute of Health Sciences, Rawalpindi, Pakistan.

College of Pharmacy, University of Sargodha Punjab, Pakistan.

出版信息

Int J Biol Macromol. 2022 Jun 30;211:425-440. doi: 10.1016/j.ijbiomac.2022.05.035. Epub 2022 May 14.

DOI:10.1016/j.ijbiomac.2022.05.035
PMID:35577197
Abstract

In current study, novel in situ formed injectable self-assembled thermoreversible depot gels based on N-(Vinylcaprolactam) were synthesized with a carbohydrate polymer i.e. sodium alginate in aqueous solution using cold method. The prepared gels preparations were intended to be utilized as 5-FU delivery depot after injectable administration through subcutaneous route. The structural characterization of self-assembled gels samples were studied through FTIR. The thermal properties of newly formed gels complexes were investigated by DSC and TGA. While the morphology of gels were assessed through SEM. The tunable gelation temperatures and phase transition of optimized formulations were confirmed by tube inverting, rheology determination and optical transmittance test. Thermo and pH response was evaluated at different temperatures and in various acidic and basic buffer solutions. In vitro release experiments were conducted using Franz diffusion system to monitor the controlled delivery fashion of gels matrices. Results concluded that depot gels exhibit controlled delivery fashion with maximum release at pH 7.4 and 37 ± 2 °C. The biocompatible nature of blank gels samples was assessed by MTT assay against Vero cell lines and was found safe. While killing ability of 5-FU encapsulated gels was evaluated against HeLa (19 ± 0.22 μg/ml; 23 ± 0.55 μg/ml) and MCF-7 (21 ± 0.06 μg/ml and 22 ± 0.34 μg/ml) cancer cell lines and were found effective to kill cancer cells. Histopathological study showed that gels depot is safe with no harmful effects on major organs. The in vivo bioavailability in rabbits showed controlled release (C, 4465.78 ± 1.99 ng/ml) in comparison to free drug (C, 4883.73 ± 3.32 ng/ml) administration after subcutaneous injection.

摘要

在当前的研究中,采用冷法在水溶液中合成了基于 N-(乙烯基己内酰胺)的新型原位形成的可注射自组装温敏储库凝胶,所用的碳水化合物聚合物为海藻酸钠。将制备的凝胶制剂通过皮下途径注射给药后用作 5-FU 输送储库。通过傅里叶变换红外光谱(FTIR)对自组装凝胶样品的结构特征进行了研究。通过差示扫描量热法(DSC)和热重分析(TGA)研究了新形成的凝胶复合物的热性能。通过扫描电子显微镜(SEM)评估了凝胶的形态。通过管倒置、流变学测定和光透过率测试确认了优化配方的可调凝胶化温度和相转变。在不同温度下和不同的酸性和碱性缓冲溶液中评估了热和 pH 响应。通过 Franz 扩散系统进行了体外释放实验,以监测凝胶基质的控制释放方式。结果表明,储库凝胶在 pH 7.4 和 37±2°C 时表现出控制释放方式,释放量最大。通过对 Vero 细胞系进行 MTT 测定评估空白凝胶样品的生物相容性,发现其安全。同时,评估了包封 5-FU 的凝胶的杀伤能力,发现其对 HeLa(19±0.22μg/ml;23±0.55μg/ml)和 MCF-7(21±0.06μg/ml 和 22±0.34μg/ml)癌细胞系有效,能够杀伤癌细胞。组织病理学研究表明,凝胶储库对主要器官无不良影响,安全。在兔体内的生物利用度研究中,与皮下注射后给予游离药物(C,4883.73±3.32ng/ml)相比,显示出控释(C,4465.78±1.99ng/ml)。

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