Dual Effects of Anti-inflammatory 2-Arylpropionic Acid Derivatives on a Major Isoform of Human Liver 3α-Hydroxysteroid Dehydrogenase

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概要

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• Nonsteroidal anti-inflammatory drugs have been shown to be potent inhibitors of mammalian 3α-hydroxy-steroid dehydrogenase. Here, we report that the drugs of the 2-arylpropionic acid class act as both activators and inhibitors for a predominant isoform of the human liver enzyme which is involved in the metabolism of steroid hormones, bile acids, drug ketones and xenobiotic aromatic hydrocarbons. Flurbiprofen, fenoprofen, ibuprofen, naproxen, ketoprofen and suprofen stimulated the activity of the human enzyme (1.5-2.4-fold) at low concentrations of less than 20-100 μM, whereas at higher concentrations they inhibited the acitivity. Comparison of the effects of the structurally related compounds with the drugs revealed that the essential structure required as the activator molecule is 2-phenylpropionic acid with a hydrophobic substituent on the aromatic ring. In addition, an R-enantiomer of ibuprofen showed higher activation (3-fold) than its S-enantiomer. Kinetic analysis with respect to NADP^+ concentration indicated that R- and S-ibuprofens are nonessential activators showing binding constants of 23 and 34 μM, respectively. Neither enantiomers activated, but rather inhibited the enzyme, with Met replacing Arg-276 which has been shown to interact with the 2'-phophate of NADP^+. The inhibitions of the mutant enzyme by R- and S-ibuprofens were competitive with respect to the substrate, giving K_i values of 95 and 18 μM, respectively. The results suggest that the human liver 3α-hydroxysteroid dehydrogenase isoform possesses the two distinct sites, activator and inhibitor sites, to which anti-inflammatory 2-arylpropionates stereoselectively bind.

• 社団法人日本薬学会の論文
• 1998-11-15

著者

• HARA Akira

  Laboratory of Biological Chemistry, Department of Applied Biological Chemistry, Faculty of Agricultu

• Yamamoto Tomohiro

  Laboratory Of Biochemistry Gifu Pharmaceutical University

• Yamamoto Tomohiro

  岐阜薬科大学 生化

• Hara A

  Department Of Pathology Gifu University School Of Medicine

• SHINTANI Syunichi

  Laboratory of Biochemistry, Gifu Pharmaceutical University

• KATAGIRI Yoshihiro

  Department of Pharmacy, Gifu University Hospital

• MATSUURA Kazuya

  Laboratory of Biochemistry, Gifu Pharmaceutical University

• SHINTANI Shunichi

  Laboratory of Biochemistry, Gifu Pharmaceutical University

• MIYABE Yoshiyuki

  Gifu Prefectural Tajimi Hospital

• SUGIYAMA Tadashi

  Department of Pharmacy, Gifu University Hospital

• Yamamoto T

  Laboratory Of Biochemistry Gifu Pharmaceutical University

• Shintani Syunichi

  Laboratory Of Biochemistry Gifu Pharmaceutical University

• Hara Akira

  Laboratory Of Biochemistry Gifu Pharmaceutical University

• Hara Akira

  Department Of Pathology Gifu University School Of Medicine

• Hara A

  Department Of Tumor Pathology Gifu University Graduate School Of Medicine

• Matsuura Kazuya

  岐阜薬科大学 生化

• Hara Akira

  岐阜薬科大学

• Katagiri Yoshihiro

  Department Of Biochemistry Gifu Pharmaceutical University

• Shintani Syunichi

  Laboratory Of Biochemistry Gifu Parmaceutical University

• Hara Akira

  Laboratory Of Biochemistry And Nutritional Chemistry:(present Address)faculty Of Agriculture Meijo U

• Sugiyama Tadashi

  Department Of Applied Chemistry Faculty Of Science Tokyo University Of Science

• Matsuura Kazuya

  Biochemistry Laboratory Gifu Pharmaceutical University

• Katagiri Yoshihiro

  Deparhnent of Pharmacy Gifu University Hospital

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