首页> 外文期刊>International Journal of Food Science >Angiotensin I-Converting Enzyme Inhibitory Peptides of Chia (Salvia hispanica) Produced by Enzymatic Hydrolysis
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Angiotensin I-Converting Enzyme Inhibitory Peptides of Chia (Salvia hispanica) Produced by Enzymatic Hydrolysis

机译:酶水解法制备的正大意香(Salvia hispanica)血管紧张素I转化酶抑制肽

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Synthetic angiotensin I-converting enzyme (ACE-I) inhibitors can have undesirable side effects, while natural inhibitors have no side effects and are potential nutraceuticals. A protein-rich fraction from chia (Salvia hispanicaL.) seed was hydrolyzed with an Alcalase-Flavourzyme sequential system and the hydrolysate ultrafiltered through four molecular weight cut-off membranes (1 kDa, 3 kDa, 5 kDa, and 10 kDa). ACE-I inhibitory activity was quantified in the hydrolysate and ultrafiltered fractions. The hydrolysate was extensive (DH = 51.64%) and had 58.46% ACE-inhibitory activity. Inhibition ranged from 53.84% to 69.31% in the five ultrafiltered fractions and was highest in the <1 kDa fraction (69.31%). This fraction’s amino acid composition was identified and then it was purified by gel filtration chromatography and ACE-I inhibition measured in the purified fractions. Amino acid composition suggested that hydrophobic residues contributed substantially to chia peptide ACE-I inhibitory strength, probably by blocking angiotensin II production. Inhibitory activity ranged from 48.41% to 62.58% in the purified fractions, but fraction F1 (1.5–2.5 kDa) exhibited the highest inhibition (IC50= 3.97 μg/mL; 427–455 mL elution volume). The results point out the possibility of obtaining bioactive peptides from chia proteins by means of a controlled protein hydrolysis using Alcalase-Flavourzyme sequentional system.
机译:合成血管紧张素I转换酶(ACE-1)抑制剂可能会产生不良副作用,而天然抑制剂则没有副作用,并且可能是营养保健品。用Alcalase-Flavourzyme顺序系统水解来自奇亚(Salvia hispanicaL。)种子的富含蛋白质的馏分,并通过四个分子量截留膜(1 kDa,3 kDa,5 kDa和10 kDa)超滤水解产物。在水解产物和超滤级分中量化了ACE-1抑制活性。水解产物广泛(DH = 51.64%),并具有5​​8.46%的ACE抑制活性。在五个超滤级分中,抑制率从53.84%到69.31%,在<1kkDa级分中抑制率最高(69.31%)。鉴定出该级分的氨基酸组成,然后通过凝胶过滤色谱法纯化,并在纯化的级分中测量ACE-1抑制率。氨基酸组成表明,疏水残基可能通过阻断血管紧张素II的产生而对Chia肽ACE-I的抑制强度有重大贡献。纯化级分的抑制活性范围为48.41%至62.58%,但级分F1(1.5-2.5 kDa)表现出最高的抑制作用(IC50 = 3.97 g / mL; 427-455 mL洗脱体积)。结果指出了通过使用Alcalase-Flavourzyme序贯系统通过受控蛋白质水解从奇亚蛋白质中获得生物活性肽的可能性。

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