首页> 外文期刊>Journal of Agricultural and Food Chemistry >Binding of Aroma Compounds with Myofibrillar Proteins Modified by a Hydroxyl-Radical-lnduced Oxidative System
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Binding of Aroma Compounds with Myofibrillar Proteins Modified by a Hydroxyl-Radical-lnduced Oxidative System

机译:芳香化合物与羟自由基诱导的氧化系统修饰的肌原纤维蛋白的结合。

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The objective of this study was to investigate the influence of oxidation-induced structural modifications of myofibrillar protein on its binding ability with aroma compounds such as 2-methyl-butanal, methional, 2-pentanone, 2-heptanone, and nonanal. A method using solid-phase microextraction (SPME) combined with gas chromatography/mass spectrometry (GC/MS) was used to determine the corresponding binding ability. The binding with aroma compounds was found to be strongly affected by the oxidation levels of proteins, probably due to the varying modifications in protein structure and surface. Incubation with oxidants around or below 1 mM mainly caused the refolding of protein structure and accelerated the protein aggregation, which reduced the affinity of the aroma compounds, thus decreasing the binding ability. Nevertheless, treatment with oxidants over 2.5 mM would cause protein reaggregation, and partial degradation, and thus, the subsequent modification of protein surface properties. The aggregated protein with wrinkled surfaces favored the hydrophobic interactions with aroma compounds, forming the protein-aroma compound complex, thus enhancing the resultant binding ability as evidenced by fluorescence quenching and SPME-GC/MS analysis.
机译:这项研究的目的是研究氧化诱导的肌原纤维蛋白的结构修饰对其与香气化合物(如2-甲基-丁醛,甲基,2-戊酮,2-庚酮和壬醛)结合能力的影响。使用固相微萃取(SPME)结合气相色谱/质谱(GC / MS)的方法来确定相应的结合能力。发现与香气化合物的结合受到蛋白质氧化水平的强烈影响,这可能是由于蛋白质结构和表面的变化所致。与大约1 mM或以下的氧化剂一起温育主要引起蛋白质结构的重新折叠并加速蛋白质聚集,从而降低了香气化合物的亲和力,从而降低了结合能力。然而,用超过2.5 mM的氧化剂处理会导致蛋白质重新聚集,并部分降解,因此,随后会改变蛋白质表面性质。表面起皱的聚集蛋白促进了与芳香化合物的疏水相互作用,形成了蛋白质-香气化合物复合物,从而增强了最终的结合能力,如荧光猝灭和SPME-GC / MS分析所证明。

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