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超声增强界面吸附及大豆胰蛋白酶抑制剂失活。

Ultrasound-enhanced interfacial adsorption and inactivation of soy trypsin inhibitors.

机构信息

Sonochemistry Group, School of Chemistry, The University of Melbourne, Parkville, Victoria 3010, Australia.

Algal Processing Group, Department of Chemical Engineering, The University of Melbourne, Parkville, Victoria 3010, Australia.

出版信息

Ultrason Sonochem. 2023 Mar;94:106315. doi: 10.1016/j.ultsonch.2023.106315. Epub 2023 Feb 2.

Abstract

In this study, liquid-liquid interfacial protein adsorption was proposed as a means of inactivating soy trypsin inhibitors (TIs, including Kunitz (KTI) and Bowman-Birk inhibitor (BBI)). Hexane-water was first selected as a model system to compare three emulsification methods (hand shaking, rotor-stator and ultrasound mixing). Ultrasound could generate the smallest and least polydisperse emulsion droplets, resulting in highest interfacial adsorption amount of KTI and BBI as well as the highest inactivation percentage of TIs (p < 0.05). Therefore, ultrasound was selected to further explore the effect of the non-aqueous phase on interfacial adsorption and inactivation kinetics of TIs in a food emulsion system containing vegetable oil (VTO). The adsorption amounts of KTI and BBI in the VTO-aqueous emulsion increased by ∼ 25 % compared to the hexane-aqueous emulsion. In addition, the adsorption amounts of KTI and BBI were rapidly increased as a function of sonication time, especially for the hexane-aqueous emulsion system. This result suggests that such inactivation of TIs could be implemented in continuous systems for large-scale processing. Finally, the pathways of interface-induced inactivation of BBI and KTI were investigated based on separate experiments on individual BBI and KTI systems. The results showed that the interface adsorption caused the changes in the secondary and tertiary structure of KTI that led to its activitation. However, BBI was quite stable at the liquid-liquid interface without significant conformational change. Overall, ultrasound-assisted interfacial adsorption can be considered a rapid and highly efficient method to inactivate KTI.

摘要

在这项研究中,提出了液-液界面蛋白吸附作为一种使大豆胰蛋白酶抑制剂(TI,包括 Kunitz(KTI)和 Bowman-Birk 抑制剂(BBI)失活的方法。首先选择正己烷-水作为模型体系,比较了三种乳化方法(手动摇晃、转子-定子和超声混合)。超声可以产生最小和最单分散的乳液液滴,导致 KTI 和 BBI 的界面吸附量最高,以及 TI 的失活百分比最高(p<0.05)。因此,选择超声进一步研究非水相在含有植物油(VTO)的食品乳液体系中对 TI 的界面吸附和失活动力学的影响。与正己烷-水乳液相比,KTI 和 BBI 在 VTO-水乳液中的吸附量增加了约 25%。此外,KTI 和 BBI 的吸附量随超声时间的增加而迅速增加,尤其是在正己烷-水乳液体系中。这一结果表明,这种 TI 的失活可以在连续系统中实施,以进行大规模处理。最后,根据单独的 BBI 和 KTI 体系的实验,研究了界面诱导 BBI 和 KTI 失活的途径。结果表明,界面吸附导致 KTI 的二级和三级结构发生变化,从而使其激活。然而,BBI 在液-液界面上相当稳定,没有明显的构象变化。总的来说,超声辅助界面吸附可以被认为是一种快速高效的方法来失活 KTI。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/f40d/9932488/a176409ad12e/ga1.jpg

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