KINETIC-STUDIES OF THE INHIBITION OF A HUMAN LIVER 3-ALPHA-HYDROXYSTEROID/DIHYDRODIOL DEHYDROGENASE ISOZYME BY BILE-ACIDS AND ANTIINFLAMMATORY DRUGS

被引:0
|
作者
MIYABE, Y
AMANO, T
DEYASHIKI, Y
HARA, A
TSUKADA, F
机构
[1] GIFU PHARMACEUT UNIV, GIFU 502, JAPAN
[2] TOKYO TANABE CO LTD, KITA KU, TOKYO 115, JAPAN
来源
BIOLOGICAL & PHARMACEUTICAL BULLETIN | 1995年 / 18卷 / 01期
关键词
ANTIINFLAMMATORY DRUG; BINDING SITE; BILE ACID; DIHYDRODIOL DEHYDROGENASE; HUMAN LIVER; KINETIC MECHANISM;
D O I
暂无
中图分类号
R9 [药学];
学科分类号
1007 ;
摘要
We have investigated the steady-state kinetics for a cytosolic 3 alpha-hydroxysteroid/dihydrodiol dehydrogenase isozyme of human liver and its inhibition by several bile acids and anti-inflammatory drugs such as indomethacin, flufemanic acid and naproxen. Initial velocity and product inhibition studies performed in the NADP(+)-linked (S)-1-indanol oxidation at pH 7.4 were consistent with a sequential ordered mechanism in which NADP(+) binds first and leaves last. The bile acids and drugs, competitive inhibitors with respect to the alcohol substrate, exhibited uncompetitive inhibition with respect to the coenzyme, with K-i values less than 1 mu M, whereas indomethacin exhibited noncompetitive inhibition (K-i<24 mu M). The kinetics of the inhibition by a mixture of the two inhibitors suggests that bile acids and drugs, except indomethacin, bind to overlapping sites at the active center of the enzyme-coenzyme binary complex.
引用
收藏
页码:9 / 12
页数:4
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