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通过工程化细胞基微结构来研究结构复杂性对脂溶性生物活性化合物生物利用度的影响。

Engineering cell-based microstructures to study the effect of structural complexity on bioaccessibility of a lipophilic bioactive compound.

机构信息

Department of Food Science and Technology, University of California-Davis, Davis, CA 95616, USA.

Department of Biological and Agricultural Engineering, University of California-Davis, Davis, CA 95616, USA.

出版信息

Food Funct. 2022 Jun 20;13(12):6560-6573. doi: 10.1039/d2fo00533f.

Abstract

A fundamental understanding of the influence of food microstructures on the bioaccessibility of micronutrients is vital for the design of functionally efficient foods. This study investigated the effect of microstructural features of model foods on the bioaccessibility of a bioactive compound - curcumin, using a unique bottom-up approach. In this approach, individual yeast cells with infused curcumin were coated with oppositely charged polyelectrolytes: first in poly(diallyl-dimethylammonium chloride), then in dextran sulfate or alginate, and assembled electrostatically to generate two types of cell clusters. These cell clusters were embedded in an alginate film to form a tissue-like structure. The influence of cell clustering and extracellular matrix on the release of encapsulated curcumin from cell-based microcarriers during simulated digestion was evaluated. Cell clusters that maintained their integrity during simulated digestion retained up to twice as much curcumin upon addition of the simulated intestinal fluid (SIF) compared to single cells during the first hour of intestinal digestion. Despite significant differences in the release profile, no spatial heterogeneity of curcumin release across a cell cluster was observed with the imaging measurements. Embedding single cells or cell clusters in calcium-crosslinked alginate films resulted in another 20-30% increase in curcumin retention and a prolonged barrier effect for more than 2 hours compared to microstructures without the films. This bottom-up approach of engineering cell-based tissue-like structures proves to be an effective method for investigating the contributions of microstructural properties of food matrices to influencing bioaccessibility of bioactives and guides future development of functional food materials.

摘要

深入了解食物微观结构对微量营养素生物可及性的影响对于设计功能高效食品至关重要。本研究采用独特的自下而上的方法,研究了模型食品的微观结构特征对生物活性化合物-姜黄素生物利用度的影响。在这种方法中,用姜黄素浸润的单个酵母细胞首先用带相反电荷的聚电解质进行涂层:首先是聚(二烯丙基二甲基氯化铵),然后是葡聚糖硫酸盐或海藻酸钠,并通过静电组装生成两种类型的细胞簇。这些细胞簇被嵌入海藻酸钠膜中以形成组织样结构。评估了细胞聚集和细胞外基质对模拟消化过程中基于细胞的微载体中封装姜黄素释放的影响。在模拟消化过程中保持完整性的细胞簇在添加模拟肠液(SIF)后保留的姜黄素高达单细胞的两倍,而在肠消化的第一个小时内则保留的姜黄素高达单细胞的两倍。尽管释放曲线存在显著差异,但通过成像测量并未观察到细胞簇中姜黄素释放的空间异质性。将单个细胞或细胞簇嵌入钙交联海藻酸钠膜中,与没有膜的微结构相比,可使姜黄素保留率增加 20-30%,并且屏障效应延长超过 2 小时。这种基于细胞的组织样结构的自下而上的工程方法被证明是一种有效的方法,可以研究食品基质的微观结构特性对影响生物活性物质生物利用度的贡献,并指导功能性食品材料的未来发展。

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