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Ellagic acid and its methyl-derivatives inhibit a newly found nitratase activity

机译:鞣花酸及其甲基衍生物抑制新发现的硝化酶活性

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We have recently shown that low density Iipoprotein (LDL) was able to denitrate albumin-bound 3-NO_2-Tyr residues and to concomitantly release NO_3~- through a Ca~(2+)-dependent process that has been ascribed to a specific protein structure. A lipophilic food component (gamma-tocopherol), which is easily loaded into LDL has been found to totally inhibit denitrating activity. We presently found that ellagic acid (EA) and its methylated derivatives, 4,4'O-methyl- and 3,3'O-methyl-ellagic acids (MeEA1 and MeEA2, respectively), amphipathic phenolic components of certain fruits and beverages, were also able to inhibit this activity, with a total inhibition for EA and a 60% inhibition for MeEA1 and MeEA2. EA exhibited the highest affinity for protein plasma, whereas a higher affinity of MeEA1 and MeEA2 (with MeEA1 > MeEA2) than EA was found for lipoprotein fractions, suggesting that the inhibition-driving property is protein affinity. As a result of this nitratase-inhibition property EA and its natural metabolite MeEA2 may have a beneficial role in special physiopathological conditions.
机译:我们最近发现,低密度脂蛋白(LDL)能够脱清白蛋白结合的3-NO_2-Tyr残基,并通过归因于特定蛋白的Ca〜(2+)依赖性过程伴随释放NO_3〜-。结构体。已发现易于装载到LDL中的亲脂性食物成分(γ-生育酚)完全抑制反硝化活性。我们目前发现,鞣花酸(EA)及其甲基化衍生物4,4'O-甲基-和3,3'O-甲基-亚麻酸(分别为MeEA1和MeEA2)是某些水果和饮料中的两亲酚类成分,它们也能够抑制这种活性,对EA的总抑制率对MeEA1和MeEA2的抑制率为60%。 EA对蛋白质血浆表现出最高的亲和力,而对于脂蛋白组分,MeEA1和MeEA2(MeEA1> MeEA2)的亲和力高于EA,这表明抑制驱动特性是蛋白质亲和力。由于具有这种硝化酶抑制特性,EA及其天然代谢产物MeEA2在特殊的生理病理条件下可能具有有益的作用。

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