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通过人工消化系统评估冷冻保护剂对作为新型口服给药系统的冻干重组酵母的活力和活性的影响。

Effects of cryoprotectants on the viability and activity of freeze dried recombinant yeasts as novel oral drug delivery systems assessed by an artificial digestive system.

作者信息

Blanquet Stéphanie, Garrait Ghislain, Beyssac Erick, Perrier Céline, Denis Sylvain, Hébrard Géraldine, Alric Monique

机构信息

Equipe de Recherche Technologique Conception, Ingénierie et Développement de l'Aliment et du Médicament (ERT CIDAM), Centre de Recherche en Nutrition Humaine (CRNH) d'Auvergne, Faculté de Pharmacie, Université d'Auvergne, Clermont-Ferrand, France.

出版信息

Eur J Pharm Biopharm. 2005 Sep;61(1-2):32-9. doi: 10.1016/j.ejpb.2005.03.009.

Abstract

The aim of this study was to investigate, in a gastric-small intestinal system TIM-1, the effect of cryoprotectants on the survival of freeze-dried Saccharomyces cerevisiae expressing the heterologous P450 73A1 and their ability to convert trans-cinnamic acid into p-coumaric acid. Yeasts were lyophilized in suspensions of trehalose, maltose, lactose, or a milk proteins/trehalose mix. Freeze-dried or native yeasts and trans-cinnamic acid were introduced simultaneously into TIM-1 at the beginning of digestion. Yeast survival rate was evaluated by cell counting in the ileal effluents. P450 73A1 activity was followed by HPLC assay of p-coumaric acid. Freeze-dried yeasts showed high tolerance to digestive conditions. Nevertheless, their survival rate was lower than that of non-dried cells (around 80% whatever the protective agent vs. 96%). The ability of recombinant freeze-dried S. cerevisiae to perform a bioconversion reaction in the digestive tract was shown with all the protectants. The highest trans-cinnamic acid conversion rate (24 vs. 41% for native yeasts) was obtained with the milk proteins/trehalose mix. These results show that freeze-drying might be considered for the pharmaceutical formulation of new drug delivery systems based on orally administered recombinant yeasts and that TIM-1 could be a helpful tool for the pre-screening of oral dosage forms.

摘要

本研究的目的是在胃-小肠系统TIM-1中,研究冷冻保护剂对表达异源细胞色素P450 73A1的冻干酿酒酵母存活率的影响,以及它们将反式肉桂酸转化为对香豆酸的能力。酵母在海藻糖、麦芽糖、乳糖或乳蛋白/海藻糖混合物的悬浮液中冻干。在消化开始时,将冻干或天然酵母与反式肉桂酸同时引入TIM-1。通过回肠流出物中的细胞计数评估酵母存活率。通过对香豆酸的高效液相色谱分析跟踪细胞色素P450 73A1的活性。冻干酵母对消化条件表现出高度耐受性。然而,它们的存活率低于未干燥的细胞(无论使用何种保护剂,冻干酵母的存活率约为80%,而未干燥细胞为96%)。所有保护剂都表明重组冻干酿酒酵母在消化道中具有进行生物转化反应的能力。使用乳蛋白/海藻糖混合物时,反式肉桂酸的转化率最高(天然酵母为24%,冻干酵母为41%)。这些结果表明,对于基于口服重组酵母的新型药物递送系统的药物制剂,冻干可能是一种可行的方法,并且TIM-1可能是口服剂型预筛选的有用工具。

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