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壳聚糖-丙烯酸共混 pH 敏感水凝胶的制备及表征及其对维拉帕米的控制释放。

Preparation and characterization of hybrid pH-sensitive hydrogels of chitosan-co-acrylic acid for controlled release of verapamil.

机构信息

Faculty of Pharmacy, BZ University, Multan, Pakistan.

出版信息

J Mater Sci Mater Med. 2010 Oct;21(10):2805-16. doi: 10.1007/s10856-010-4134-1. Epub 2010 Aug 5.

Abstract

In the present work crosslinked hydrogels based on chitosan (CS) and acrylic acid (AA) were prepared by free radical polymerization with various feed compositions using N,N methylenebisacrylamide (MBA) as crosslinking agent. Benzoyl peroxide was used as catalyst. Fourier transform infrared spectra (FTIR) confirmed the formation of the crosslinked hydrogels. This hydrogel is formed due to electrostatic interaction between cationic groups in CS and anionic groups in AA. Prepared hydrogels were used for dynamic and equilibrium swelling studies. For swelling behavior, effect of pH, polymeric and monomeric compositions and degree of crosslinking were investigated. Swelling studies were performed in USP phosphate buffer solutions of varying pH 1.2, 5.5, 6.5 and 7.5. Results showed that swelling increased by increasing AA contents in structure of hydrogels in solutions of higher pH values. This is due to the presence of more carboxylic groups available for ionization. On the other hand by increasing the chitosan content swelling increased in a solution of acidic pH, but this swelling was not significant and it is due to ionization of amine groups present in the structure of hydrogel. Swelling decreased with increase in crosslinking ratio owing to tighter hydrogel structure. Porosity and sol-gel fraction were also measured. With increase in CS and AA contents porosity and gel fraction increased, whereas by increasing MBA content porosity decreased and gel fraction increased. Furthermore, diffusion coefficient (D) and the network parameters i.e., the average molecular weight between crosslinks (M(c)), polymer volume fraction in swollen state (V(2s)), number of repeating units between crosslinks (M(r)) and crosslinking density (q) were calculated using Flory-Rehner theory. Selected samples were loaded with a model drug verapamil. Release of verapamil depends on the ratios of CS/AA, degree of crosslinking and pH of the medium. The release mechanisms were studied by fitting experimental data to model equations and calculating the corresponding parameters. The result showed that the kinetics of drug release from the hydrogels in both pH 1.2 and 7.5 buffer solutions was mainly non-Fickian diffusion.

摘要

在本工作中,通过自由基聚合,以不同的进料组成,使用 N,N-亚甲基双丙烯酰胺(MBA)作为交联剂,制备了壳聚糖(CS)和丙烯酸(AA)的交联水凝胶。用过氧化苯甲酰作为催化剂。傅里叶变换红外光谱(FTIR)证实了交联水凝胶的形成。这种水凝胶是由于 CS 中的阳离子基团和 AA 中的阴离子基团之间的静电相互作用形成的。制备的水凝胶用于动态和平衡溶胀研究。对于溶胀行为,研究了 pH 值、聚合物和单体组成以及交联度的影响。在不同 pH 值的 USP 磷酸盐缓冲溶液中进行了溶胀研究 1.2、5.5、6.5 和 7.5。结果表明,在较高 pH 值的溶液中,通过增加水凝胶结构中的 AA 含量,溶胀增加。这是由于存在更多可用于电离的羧酸基团。另一方面,通过增加壳聚糖含量,在酸性 pH 值溶液中溶胀增加,但这种溶胀不明显,这是由于水凝胶结构中存在的胺基的电离。由于水凝胶结构更紧密,交联比增加导致溶胀减少。还测量了孔隙率和溶胶-凝胶分数。随着 CS 和 AA 含量的增加,孔隙率和凝胶分数增加,而随着 MBA 含量的增加,孔隙率降低,凝胶分数增加。此外,使用 Flory-Rehner 理论计算了扩散系数(D)和网络参数,即交联平均分子量(M(c))、溶胀状态下聚合物体积分数(V(2s))、交联重复单元数(M(r))和交联密度(q)。选择了一些样品进行维拉帕米的模型药物负载。维拉帕米的释放取决于 CS/AA 的比例、交联度和介质的 pH 值。通过将实验数据拟合到模型方程并计算相应的参数来研究释放机制。结果表明,在 pH 1.2 和 7.5 缓冲溶液中,水凝胶中药物释放的动力学主要是非菲克扩散。

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