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蛋白质稳定乳液的界面设计,以实现最佳的营养传递。

Interfacial design of protein-stabilized emulsions for optimal delivery of nutrients.

机构信息

Department of Food Science, University of Guelph, Guelph, Ontario, Canada.

出版信息

Food Funct. 2010 Nov;1(2):141-8. doi: 10.1039/c0fo00099j. Epub 2010 Oct 5.

Abstract

Proteins are often used as ingredients in food emulsions, as their amphiphilic structures provide electrostatic and steric stabilization. Significant attention has recently been directed at understanding how the composition and structure of oil-water interfaces change during digestion and how these can be manipulated to enhance the delivery of nutrients contained within the oil droplets. These efforts have necessitated the development of more sophisticated in vitro digestion models of greater physiological relevance and increased efforts in research to identify the role of the various digestive parameters on interfacial dynamics. The changes occurring at the oil-water interface will affect the adsorption of gastro-intestinal lipases and, ultimately, affect lipid digestion. The composition of a protein-stabilized oil droplet changes continuously during digestion, because of proteolysis and the formation of peptides with different affinities for the interface. In addition, natural bio-surfactants such as phospholipids and bile salts, other surface- active molecules present in foods, and the products of lipolysis (i.e. mono and diglycerides, lysophospholipids), all compete for access to the interface, and contribute to the dynamic changes occurring on the surface of the oil droplets. A better understanding of how to tailor the composition of oil droplet surfaces in food emulsions will aid in optimizing lipid digestion and, as a result, delivery of lipophilic nutrients. This review focuses on the physico-chemical changes occurring in protein-stabilized oil-in-water emulsions during gastric and small intestine digestion, and on how interfacial engineering could lead to differences in fatty acid release and the potential bioavailability of lipophilic molecules.

摘要

蛋白质通常被用作食品乳液的成分,因为它们的两亲结构提供了静电和空间稳定作用。最近,人们对理解油-水界面在消化过程中的组成和结构如何变化以及如何操纵这些变化以增强油滴内所含营养物质的传递给予了极大关注。这些努力需要开发更复杂的具有更高生理相关性的体外消化模型,并增加研究力度以确定各种消化参数对界面动力学的作用。油-水界面发生的变化将影响胃肠脂肪酶的吸附,最终影响脂肪消化。由于蛋白质稳定的油滴在消化过程中不断发生蛋白质水解和形成具有不同界面亲和力的肽,其组成会发生变化。此外,天然生物表面活性剂(如磷脂和胆汁盐)、食品中存在的其他表面活性分子以及脂肪分解的产物(即单甘酯和二甘酯、溶血磷脂)都会竞争进入界面,导致油滴表面发生动态变化。更好地了解如何调整食品乳液中油滴表面的组成将有助于优化脂肪消化,从而提高脂溶性营养素的生物利用度。本综述重点介绍了在胃和小肠消化过程中,蛋白质稳定的油包水乳状液中发生的物理化学变化,以及界面工程如何导致脂肪酸释放和脂溶性分子潜在生物利用度的差异。

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