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黄酮类化合物槲皮素与人血清白蛋白形成复合物后对亚油酸过氧化的抑制作用。

Inhibition of the peroxidation of linoleic acid by the flavonoid quercetin within their complex with human serum albumin.

作者信息

Dufour Claire, Loonis Michèle, Dangles Olivier

机构信息

UMR408 Sécurité et Qualité des Produits d'Origine Végétale, INRA, Université d'Avignon, Domaine St Paul, Site Agroparc, 84914 Avignon, France.

出版信息

Free Radic Biol Med. 2007 Jul 15;43(2):241-52. doi: 10.1016/j.freeradbiomed.2007.04.009. Epub 2007 Apr 14.

Abstract

This work provides a quantitative kinetic analysis of oxidative pathways involving linoleic acid and the common dietary antioxidant quercetin (flavonoid), both bound to human serum albumin (HSA). In particular, it is shown that quercetin, although embedded in drug site I, is oxidized as quickly as free quercetin under a flux of hydrophilic peroxyl radicals. This observation suggests that efficient charge relays are established between the periphery of HSA and bound quercetin. Moreover, the peroxidation of HSA-bound linoleic acid is shown to take place at some specific fatty acid binding sites once one to two critical HSA residues are themselves oxidized. Quercetin efficiently delays the onset of lipid peroxidation. The inhibition persists long after the total consumption of quercetin, in agreement with some quercetin oxidation products exerting a residual antioxidant activity. Consistently, HSA markedly increases the maximal concentration of a two-electron oxidation product of quercetin that is accumulated and then consumed in the course of the peroxidation. The additional observation of the faster consumption of the single Trp residue in the presence of quercetin suggests that HSA enhances the antioxidant activity of quercetin by regenerating some of its oxidation products retaining a H-donating activity.

摘要

这项工作对涉及亚油酸和常见膳食抗氧化剂槲皮素(类黄酮)的氧化途径进行了定量动力学分析,二者均与人血清白蛋白(HSA)结合。具体而言,研究表明,尽管槲皮素嵌入药物位点I,但在亲水性过氧自由基通量下,其氧化速度与游离槲皮素一样快。这一观察结果表明,在HSA的外围和结合的槲皮素之间建立了有效的电荷中继。此外,一旦一到两个关键的HSA残基自身被氧化,与HSA结合的亚油酸的过氧化作用就会在一些特定的脂肪酸结合位点发生。槲皮素能有效延迟脂质过氧化的发生。在槲皮素完全消耗后很长时间,这种抑制作用仍然存在,这与一些槲皮素氧化产物具有残留抗氧化活性一致。同样,HSA显著增加了槲皮素双电子氧化产物的最大浓度,该产物在过氧化过程中积累然后消耗。在槲皮素存在的情况下,单个色氨酸残基消耗更快这一额外观察结果表明,HSA通过再生一些保留H供体活性的氧化产物来增强槲皮素的抗氧化活性。

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