S Koizumi, T Nagatsu, H Iinuma, M Ohno, T Takeuchi, H Umezawa
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引用次数: 7
摘要
苯丙氨酸羟化酶在体外实验中被证实受到欧地酮及其衍生物的抑制。在2.3 x 10(-3) M的浓度下,乌德酮对苯丙氨酸羟化酶的抑制作用达到50%,某些乌德酮衍生物的抑制作用更强。动力学数据表明,甾酮对四氢蝶呤辅助因子(6,7-二甲基四氢蝶呤,DMPH4)的抑制是竞争性的,而对苯丙氨酸和氧的抑制是非竞争性的。12种甾酮衍生物对苯丙氨酸羟化酶的抑制作用与酪氨酸羟化酶的抑制作用没有平行的构效关系。欧德酮的衍生物,[化合物142];2-(3,4-二羟基苯基)-1-氧丙基)环己烷-1,3-二酮]对甾酮类化合物的抑制作用最强。在1.8 x 10(-5) m的浓度下,对苯丙氨酸羟化酶的抑制作用为50%。这种抑制作用与四氢蝶呤辅助因子DMPH4或底物苯丙氨酸的抑制作用是混合型的,与欧地酮的抑制作用不同。然而,同样的非竞争性抑制也表现为对氧的抑制。
Inhibition of phenylalanine hydroxylase, a pterin-requiring monooxygenase, by oudenone and its derivatives.
Phenylalanine hydroxylase was shown to be inhibited by oudenone and its derivatives in vitro. At a concentration of 2.3 x 10(-3) M, oudenone inhibited phenylalanine hydroxylase by 50%, and some of the oudenone derivatives showed more potent inhibition. The kinetic data have shown that the inhibition by oudenone is competitive with a tetrahydropterin cofactor (6,7-dimethyltetrahydropterin, DMPH4) and noncompetitive with phenylalanine and oxygen. Among 12 oudenone derivatives, there was no parallel structure-activity relationship between the inhibitory effect for phenylalanine hydroxylase and that for tyrosine hydroxylase. A derivative of oudenone, [compound No. 142; 2-(3,4-dihydroxyphenyl)-1-oxopropyl)cyclohexan-1,3-dione] showed the most potent inhibition among the oudenone derivatives. It inhibited phenylalanine hydroxylase by 50% at a concentration of 1.8 x 10(-5) M. This inhibition was a mixed type with either a tetrahydropterin cofactor, DMPH4, or with the substrate phenylalanine, which was different from the inhibition by oudenone. However, the same noncompetitive inhibition was shown toward oxygen.
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