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Synthesis, in vitro and cellular antioxidant activity evaluation of novel peptides derived from Saccharomyces cerevisiae protein hydrolysate: structure-function relationship Antioxidant activity and synthetic peptides

机译:合成,体外和细胞抗氧化活性评价衍生自酿酒酵母蛋白水解产物的新型肽:结构功能关系抗氧化活性和合成肽

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摘要

The relationship between structure and function of primary antioxidant peptide, YR-10 (YGKPVAVPAR) was considered by synthesizing three analogues including YHR-10 (YGKHVAVHAR), GA-8 (GKPVAVPA) and PAR-3 (PAR). Antioxidant activity was determined through in vitro and cellular assays. Substitution of Pro with His in the structure of YR-10 led to significant (P < 0.05) higher ABTS radical scavenging and ferric reducing activity. Following in silico simulated gastrointestinal digestion, Tyr and Arg were omitted, respectively, from N and C-terminal positions and resulted in decreasing DPPH, ABTS radical scavenging, and ferric reducing activities. PAR-3 showed the best inhibitory activity on linoleic acid oxidation. Pretreatment of Caco-2 cells with YR-10, YHR-10, and GA-8 (1000 mu M) before exposure to H2O2 (160 mu M) resulted in 34.10%, 39.66% and 29.159% reduction in malondialdehyde and 53.52%, 17.02% and 24.71% reduction in protein carbonyl levels. The peptide pretreatment reduced catalase level in cells and PAR-3 exhibited the most protective effects on the viability of cells exposed to oxidative stress.
机译:通过合成包括YHR-10(YGKHVAVHAR),GA-8(GKPVAVPA)和PAR-3(PAR)的三种类似物来考虑原发性抗氧化肽的结构和功能的关系。通过体外和细胞测定法测定抗氧化活性。 Pro用他的YR-10结构替换为显着(P <0.05),高级ABTS激进清除和菲克减少活性。在Silico模拟胃肠道消化中,分别从N和C末端位置省略Tyr和Arg,导致DPPH,ABTS自由基清除和还原活性降低。 PAR-3显示了亚油酸氧化的最佳抑制活性。在暴露于H 2 O 2(160μm)之前,用YR-10,YHR-10和Ga-8(1000μm)的预处理在H 2 O 2(160μm)之前,导致丙二醛的减少34.10%,39.66%和29.159%,53.52%,蛋白质羰基水平降低17.02%和24.71%。肽预处理降低细胞中的过氧化氢酶水平,并且PAR-3对暴露于氧化应激的细胞的活力表现出最具保护性的影响。

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