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Structure and shelf stability of milk protein gels created by pressure-assisted enzymatic gelation

机译:压力辅助酶凝胶产生的牛奶蛋白凝胶的结构和货架稳定性

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In this work, pressure-assisted enzymatic gelation was applied to milk proteins, with the goal of enhancing the structure and stability of pressure-created milk protein gels. High-pressure processing (HPP) at 600 MPa, 3 min, and 5°C was applied to milk protein concentrate (MPC) samples of 12.5% protein concentration, both in the absence and in the presence of calf chymosin [up to 60 IMCU (international milk-clotting units)/kg of milk] or camel chymosin (up to 45 IMCU/ kg of milk). Gel hardness, water-holding capacity, and degree of proteolysis were used to assess network strength and shelf stability. The processing trials and all measurements were conducted in triplicate. Statistical analyses of the data were performed by ANOVA, at a 95% confidence level. After HPP treatment, we observed significant structural changes for all samples. Pressurization of MPC, with or without chymosin addition, led to extensive protein aggregation and network formation. The strength of HPP-created milk protein gels without chymosin addition, as measured by the elastic modulus (G′), had a value of 2,242 Pa. The value of G′ increased with increasing chymosin concentration, reaching as high as 4,800 Pa for samples with 45 IMCU/kg of camel chymosin. During 4 wk of refrigerated storage, the HPP and chymosin MPC gels maintained higher gel hardness and better structural stability compared with HPP only (no chymosin) MPC gels. The water-holding capacity of the gels without chymosin remained at 100% during 28 d of refrigerated storage. The HPP and chymosin MPC gels had a lower water-holding capacity (91-94%) than the HPP-only counterparts, but their water-holding capacity did not decrease during storage. Overall, these findings demonstrate that controlled, fast structural modification of high-concentration protein systems can be obtained by HPP-assisted enzymatic treatment, and the created gels have a strong, stable network. This study provides insights into the possibility of using HPP for the development of milk-protein-based products with novel structures and textures and long refrigerated shelf life, along with the built-in safety imparted by the HPP treatment.
机译:在这项工作中,将压力辅助的酶促凝胶化应用于乳蛋白,目的是提高压力产生的乳蛋白凝胶的结构和稳定性。在600MPa,3分钟和5℃下施加高压处理(HPP),施加到牛奶蛋白浓缩物(MPC)样品为12.5%蛋白质浓度的样品,无论是在缺失和牛犊的情况下,都在牛皮蛋白酶的情况下[达60μc (国际牛奶凝块单位)/ kg牛奶]或骆驼chymosin(最多45个IMCU / kg牛奶)。使用凝胶硬度,水持能力和蛋白水分程度来评估网络强度和货架稳定性。加工试验和所有测量一式三份进行。数据的统计分析由ANOVA进行95%的置信水平。在HPP治疗后,我们观察到所有样品的显着结构变化。 MPC的加压,有或没有唇息素的添加,导致了广泛的蛋白质聚集和网络形成。通过弹性模量(g')测量的HPP产生的乳蛋白凝胶的强度具有2,242Pa的值。增加了肠蛋白浓度的增加值,达到4,800Pa的样品用45个IMCU / kg骆驼胰蛋白酶。在4WK的冷藏储存期间,与仅与HPP(无底皮蛋白)MPC凝胶相比,HPP和胰蛋白酶MPC凝胶保持较高的凝胶硬度和更好的结构稳定性。在28 d冷藏储存期间,没有乳糜蛋白的凝胶的水持续容量保持在100%。 HPP和胰蛋白酶MPC凝胶的水持量较低(91-94%),而不是仅用于HPP的对应物,但在储存期间它们的水持续物容量不会降低。总体而言,这些研究结果表明,通过HPP辅助酶促处理可以获得受控的,快速结构改性,并且产生的凝胶具有强,稳定的网络。本研究提供了利用HPP为开发具有新型结构和纹理和长冷藏保质期的牛奶蛋白的产品的可能性的见解,以及通过HPP处理赋予的内置安全性。

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