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生产过程以及胃/肠道模拟过程中影响藻酸盐-壳聚糖凝聚微胶囊蛋白质释放的因素

Factors affecting protein release from alginate-chitosan coacervate microcapsules during production and gastric/intestinal simulation.

作者信息

Vandenberg G W, Drolet C, Scott S L, de la Noüe J

机构信息

Groupe de recherche en recyclage biologique et aquiculture. Département des sciences animales, Université Laval, Pavillon Paul Comtois, Ste-Foy, G1K-7P4, Québec, Canada.

出版信息

J Control Release. 2001 Dec 13;77(3):297-307. doi: 10.1016/s0168-3659(01)00517-x.

Abstract

A series of experiments was performed to evaluate the influence of a number of physico-chemical factors on the diffusion of a model protein, bovine serum albumin (BSA), from dried chitosan-coated alginate microcapsules. Diffusion of BSA was quantified during the microcapsule manufacture processes (gelation, washing, rinsing) and during incubation in conditions simulating the pH encountered during the gastric (0.1 N HCl; pH 1.5) and intestinal (200 mM Tris-HCl; pH 7.5) phases of digestion. Factors tested included alginate and chitosan concentration, calcium chloride (CaCl2) concentration in the gelation medium, loading rate, chitosan molecular mass and pH of the gelation medium. Microcapsule size and gelation time were altered in order to determine their effects on protein retention. Alginate and chitosan concentration significantly influenced BSA retention during microcapsule manufacture and acid incubation, as did calcium chloride concentration in the gelation medium (P<0.05). BSA retention during manufacture was not significantly altered by protein loading rate or pH of the encapsulation medium, however, protein retention during acid incubation decreased significantly with increasing protein loading rate and encapsulation medium pH (P<0.05). Microcapsules that were washed with acetone following manufacture demonstrated significantly increased protein retention during acid incubation (P<0.05). In microcapsules that had been acetone-dried to a point whereby their mass was reduced to 10% of that immediately following encapsulation, protein retention was over 80% following 24-h acid incubation vs. only 20% protein retention from non acetone-dried microcapsules. The presence of calcium in the neutral buffer medium significantly reduced BSA diffusion in a concentration-dependent manner (P<0.05).

摘要

进行了一系列实验,以评估多种物理化学因素对模型蛋白牛血清白蛋白(BSA)从干燥的壳聚糖包被藻酸盐微胶囊中扩散的影响。在微胶囊制造过程(凝胶化、洗涤、冲洗)以及模拟胃(0.1 N HCl;pH 1.5)和肠(200 mM Tris-HCl;pH 7.5)消化阶段所遇到的pH条件下孵育期间,对BSA的扩散进行了定量。测试的因素包括藻酸盐和壳聚糖浓度、凝胶化介质中的氯化钙(CaCl2)浓度、负载率、壳聚糖分子量以及凝胶化介质的pH。改变微胶囊尺寸和凝胶化时间以确定它们对蛋白质保留的影响。藻酸盐和壳聚糖浓度在微胶囊制造和酸孵育期间对BSA保留有显著影响,凝胶化介质中的氯化钙浓度也是如此(P<0.05)。制造过程中BSA的保留不受蛋白质负载率或包封介质pH的显著影响,然而,随着蛋白质负载率和包封介质pH的增加,酸孵育期间的蛋白质保留显著降低(P<0.05)。制造后用丙酮洗涤的微胶囊在酸孵育期间显示出蛋白质保留显著增加(P<0.05)。在已用丙酮干燥至其质量降至包封后立即质量的10%的微胶囊中,24小时酸孵育后蛋白质保留率超过80%,而非丙酮干燥的微胶囊蛋白质保留率仅为20%。中性缓冲介质中钙的存在以浓度依赖的方式显著降低了BSA的扩散(P<0.05)。

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