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基于纤维素和壳聚糖的通过同时双重点击策略制备的热/pH 响应性互穿网络水凝胶药物载体的简便制备方法。

Facile fabrication of a thermal/pH responsive IPN hydrogel drug carrier based on cellulose and chitosan through simultaneous dual-click strategy.

机构信息

School of Chemistry and Chemical Engineering, Henan University of Technology, Zhengzhou, PR China.

The Key Laboratory of Biomedical Material, School of Life Science and Technology, Xinxiang Medical University, Xinxiang, PR China.

出版信息

J Colloid Interface Sci. 2025 Jan 15;678(Pt A):827-841. doi: 10.1016/j.jcis.2024.08.208. Epub 2024 Aug 28.

Abstract

Herein, an interpenetrating network hydrogel (IPN-Gel) based on cellulose and chitosan was synthesized via simultaneous amino-anhydride and azide-alkyne click reaction in water in one pot. The samples were characterized by various analytical methods including FTIR, SEM, XRD, XPS, H NMR and so forth. The fabrication conditions were optimized by single factor experiments with water uptake (WU) and gel mass fraction (GMF) as two indexes. The WU and GMF of the IPN-Gel prepared under optimized conditions were 1192.37 % and 74.00 %, respectively. Its WU descended with the ascension in temperature, and first descended and then gradually ascended with the ascension in pH, confirming that the IPN-Gel had thermal/pH dual responsiveness. Using 5-Fu as a model drug, the release behavior of 5-Fu in IPN-Gel was explored. Its release behavior could be regulated by changing temperature and pH values, and it followed the Korsmeyer Peppas model. The viability of 4 T1 cells and HUVEC cells exceeded 80 % after 48 h of incubation at a high concentration of 200 μg/mL IPN-Gel, and hemolytic percentage was below the allowed limit of 5 %. The study provides a new strategy for the preparation of the IPN-Gel with biocompatibility, swelling reversibility and controllable drug release.

摘要

本文通过在一锅法中同时进行氨基-酸酐和叠氮-炔基点击反应,合成了基于纤维素和壳聚糖的互穿网络水凝胶(IPN-Gel)。通过各种分析方法对样品进行了表征,包括 FTIR、SEM、XRD、XPS、H NMR 等。通过单因素实验,以吸水率(WU)和凝胶质量分数(GMF)为两个指标,优化了制备条件。在优化条件下制备的 IPN-Gel 的吸水率和凝胶质量分数分别为 1192.37%和 74.00%。其吸水率随温度升高而下降,随 pH 值升高先下降后逐渐升高,表明 IPN-Gel 具有热/pH 双重响应性。以 5-Fu 为模型药物,探讨了 5-Fu 在 IPN-Gel 中的释放行为。通过改变温度和 pH 值可以调节其释放行为,且符合 Korsmeyer-Peppas 模型。在 200μg/mL IPN-Gel 高浓度孵育 48 小时后,4T1 细胞和 HUVEC 细胞的活力超过 80%,且溶血率低于 5%的允许限值。该研究为制备具有生物相容性、溶胀可逆性和可控药物释放的 IPN-Gel 提供了一种新策略。

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