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胃内重构决定了具有不同质地的热凝乳蛋白凝胶的消化动力学。

Intragastric restructuring dictates the digestive kinetics of heat-set milk protein gels of contrasting textures.

机构信息

Riddet Institute, Massey University, Private Bag 11 222, Palmerston North 4442, New Zealand.

Smart Foods & Bioproducts Group, AgResearch Ltd, Te Ohu Rangahau Kai, Massey University, Palmerston North 4442, New Zealand.

出版信息

Food Res Int. 2024 Nov;195:114944. doi: 10.1016/j.foodres.2024.114944. Epub 2024 Aug 27.

DOI:10.1016/j.foodres.2024.114944
PMID:39277222
Abstract

The gelation of milk proteins can be achieved by various means, enabling the development of diverse products. In this study, heat-set milk protein gels (15 % protein) of diverse textures were made by pH modulation and two gels were selected for dynamic in vitro gastric digestion: a spoonable soft gel (SG, pH 6.55' G' of ∼100 Pa) and a sliceable firm gel (FG, pH 5.65; G' of ∼7000 Pa). The two gels displayed markedly different structural changes and digestion kinetics during gastric digestion. The SG underwent substantial structural compaction during the first 120 min of gastric digestion into a denser and firmer gastric chyme (26.3 % crude protein, G* of ∼8500 Pa) than the chyme of the FG (15.7 % crude protein, G* of ∼3000 Pa). These contrasting intragastric structural changes of the gels reversed their original textural differences, which led to slower digestion and gastric emptying of proteins from the SG compared with the FG. The different intragastric pH profiles during the digestion of the two gels likely played a key role by modulating the proteolytic activity and specificity (to κ-casein) of pepsin. Preferential early cleavage of κ-casein in SG stimulated coagulation and compaction of solid chyme, whereas rapid hydrolysis of α- and β-caseins in the FG weakened coagulation. This study provided new insights into controlling the structural development of dairy-based foods during gastric digestion and modulating digestion kinetics.

摘要

牛奶蛋白的胶凝可以通过各种方法实现,从而开发出各种产品。在本研究中,通过 pH 值调节制备了具有不同质地的热凝乳蛋白凝胶(15%蛋白质),并选择了两种凝胶进行动态体外胃消化研究:一种可勺取的软凝胶(SG,pH6.55'G'约为 100Pa)和一种可切片的硬凝胶(FG,pH5.65;G'约为 7000Pa)。这两种凝胶在胃消化过程中表现出明显不同的结构变化和消化动力学。SG 在胃消化的前 120 分钟内经历了显著的结构紧缩,形成了更致密和更坚硬的胃食糜(粗蛋白 26.3%,G约为 8500Pa),而 FG 的胃食糜(粗蛋白 15.7%,G约为 3000Pa)则较为疏松。凝胶的这些对比鲜明的胃内结构变化逆转了它们原有的质地差异,导致 SG 中的蛋白质消化和排空速度比 FG 更慢。两种凝胶在消化过程中不同的胃内 pH 分布可能通过调节胃蛋白酶的蛋白水解活性和特异性(κ-酪蛋白)发挥关键作用。SG 中 κ-酪蛋白的优先早期切割刺激了固体食糜的凝结和紧缩,而 FG 中 α-和 β-酪蛋白的快速水解则削弱了凝结。本研究为控制胃消化过程中乳制品的结构发展和调节消化动力学提供了新的见解。

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