首页> 美国卫生研究院文献>International Journal of Molecular Sciences >Angiotensin I-Converting Enzyme (ACE) Inhibitory Activity and ACE Inhibitory Peptides of Salmon (Salmo salar) Protein Hydrolysates Obtained by Human and Porcine Gastrointestinal Enzymes
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Angiotensin I-Converting Enzyme (ACE) Inhibitory Activity and ACE Inhibitory Peptides of Salmon (Salmo salar) Protein Hydrolysates Obtained by Human and Porcine Gastrointestinal Enzymes

机译:人和猪胃肠道酶获得的鲑鱼(Salmo salar)蛋白水解产物的血管紧张素I转换酶(ACE)抑制活性和ACE抑制肽

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摘要

The objectives of the present study were two-fold: first, to detect whether salmon protein fractions possess angiotensin I-converting enzyme (ACE) inhibitory properties and whether salmon proteins can release ACE inhibitory peptides during a sequential in vitro hydrolysis (with commercial porcine enzymes) and ex vivo digestion (with human gastrointestinal enzymes). Secondly, to evaluate the ACE inhibitory activity of generated hydrolysates. A two-step ex vivo and in vitro model digestion was performed to simulate the human digestion process. Salmon proteins were degraded more efficiently by porcine enzymes than by human gastrointestinal juices and sarcoplasmic proteins were digested/hydrolyzed more easily than myofibrillar proteins. The ex vivo digested myofibrillar and sarcoplasmic duodenal samples showed IC50 values (concentration required to decrease the ACE activity by 50%) of 1.06 and 2.16 mg/mL, respectively. The in vitro hydrolyzed myofibrillar and sarcoplasmic samples showed IC50 values of 0.91 and 1.04 mg/mL, respectively. Based on the results of in silico studies, it was possible to identify 9 peptides of the ex vivo hydrolysates and 7 peptides of the in vitro hydrolysates of salmon proteins of 11 selected peptides. In both types of salmon hydrolysates, ACE-inhibitory peptides IW, IY, TVY and VW were identified. In the in vitro salmon protein hydrolysates an ACE-inhibitory peptides VPW and VY were also detected, while ACE-inhibitory peptides ALPHA, IVY and IWHHT were identified in the hydrolysates generated with ex vivo digestion. In our studies, we documented ACE inhibitory in vitro effects of salmon protein hydrolysates obtained by human and as well as porcine gastrointestinal enzymes.
机译:本研究的目标有两个方面:首先,检测鲑鱼蛋白级分是否具有血管紧张素I转换酶(ACE)抑制特性,以及鲑鱼蛋白在连续体外水解过程中是否可以释放ACE抑制肽(使用商业猪酶) )和离体消化(使用人类胃肠道酶)。其次,评估生成的水解产物的ACE抑制活性。进行了两步体外和体外模型消化,以模拟人的消化过程。猪酶比人胃肠液更有效地降解鲑鱼蛋白,并且肌浆蛋白比肌原纤维蛋白更易于消化/水解。离体消化的肌原纤维和肌浆十二指肠样品的IC50值(使ACE活性降低50%所需的浓度)分别为1.06和2.16 mg / mL。体外水解的肌原纤维和肌浆样品的IC50值分别为0.91和1.04 mg / mL。基于计算机模拟研究的结果,有可能从11种选定的肽中鉴定出9种离体水解产物的肽和7种鲑鱼蛋白体外水解产物的肽。在两种类型的鲑鱼水解物中,均已鉴定出ACE抑制肽IW,IY,TVY和VW。在体外鲑鱼蛋白水解物中,还检测到ACE抑制肽VPW和VY,而在离体消化产生的水解物中鉴定出ACE抑制肽ALPHA,IVY和IWHHT。在我们的研究中,我们记录了人和猪胃肠道酶获得的鲑鱼蛋白水解物的ACE抑制体外作用。

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