Studies on the Interactions between Drugs and Estrogen. III. Inhibitory Effects of 29 Drugs Reported to Induce Gynecomastia on the Glucuronidation of Estradiol(Miscellaneous)
スポンサーリンク
概要
- 論文の詳細を見る
To determine the inhibition effects of drugs on the glucuronidation of estradiol (E2), 29 drugs that have been reported to induce gynecomastia were examined in the presence of UDP-glucuronic acid using human hepatic microsomes (pooled) as the enzyme source. The percentage inhibition of the E2 glucuronidation was determined at drug concentrations of 1 μM (approximate therapeutic concentration) and 100μM (non-clinical overdose concentration) based on the rate constants for the 3- and 17-glucuronidation of E2 (11.2 and 2.52 pmol/min/mg protein, respectively). The only drug that exhibited 50% or higher inhibition of the 3-glucuronidation at a concentration of 1 μM was manidipine (54.4%). When the concentration was 100 μM, manidipine exhibited 100% inhibition of the 3-glucuronidation, and other drugs that exhibited 50% or higher inhibition of the 3-glucuronidation were nicardipine (92%), nisoldipine (90%), nifedipine (84%), domperidone (81%), tacrolimus (80%), nitrendipine (77%) and ketoconazole (69%). Conversely, ipriflavone accelerated the formation of estradiol 3-glucuronide in the activity of 165% at the concentration of 100μM. On the 17-glucuronidation, all of the drugs showed less than 50% inhibition at the concentration of 1 μM, but at the concentration of 100μM, drugs that exhibited 50% or higher inhibition consisted of manidipine (79%), chlormadinone acetate (74%), nisoldipine (66%), nitrendipine (60%) and ketoconazole (55%). Although IC_<50> values of these drugs were all lower than the K_m value (285μM) for the 3-glucuronidation of E2, they were higher than the K_m value for the 17-glucuronidation (18.8 μM). Thus, the effect of the drugs on the E2 glucuronidation should be greater for hydroxy group at the C-3 than that at the C-17 of E2 molecule. On the other hand, metabolic clearances (V_<max>/K_m) of the 3- and 17-glucuronidation were about 1/14th and 1/18th of that of the 2-hydroxylation of E2, respectively. The result implies that, when the contribution of the glucuronidation to enterohepatic circulation is taken into consideration, the effect of this metabolic inhibition in the estrogen pool cannot be ignored.
- 公益社団法人日本薬学会の論文
- 2004-11-01
著者
-
伊藤 慎二
北海道薬科大学
-
伊藤 慎二
Hokkaido College Of Pharmacy
-
SATOH Takashi
Yakuhan Pharmaceutical Co., Ltd.
-
TOMIKAWA Yuki
Yakuhan Pharmaceutical Co., Ltd.
-
TAKANASHI Kaori
Hokkaido College of Pharmacy
-
ITOH Shinji
Hokkaido College of Pharmacy
-
ITOH Shungo
Japan Seamen-Relief-Association Otaru Hospital
-
YOSHIZAWA Itsuo
Hokkaido College of Pharmacy
-
ITOH Yoshimi
Hokkaido College of Pharmacy
-
Kashiwagi Tomohiro
Department Of Obstetrics And Gynecology Kyoto Prefectural University Of Medicine
-
Satoh T
Tokyo Univ. Sci. Tokyo Jpn
-
Yoshizawa I
Hokkaido College Of Pharmacy
-
Tomikawa Y
Yakuhan Pharmaceutical Co. Ltd.
-
Satoh Takashi
Yakuhan Pharmaceutical Co. Ltd.
関連論文
- D環抱合型エストロゲンの高速液体クロマトグラフィーによる一斉分離検出 ( バイオサイエンスと分析化学)
- Effect of Estrogen Replacement Therapy on Hepatic Triglyceride Lipase, Lipoprotein Lipase and Lipids Including Apolipoprotein E in Climacteric and Elderly Women
- On the Rearrangement Reactions of Pregnanediol Disulfate to Δ^-Steroid, and Its 20-Isomeric Sulfate to D-Homosteroids : Clinical Analysis on Steroids. XLII
- 5β-Pregn-20-en-3α-olのリトコール酸からの合成
- 5β-Pregnane-3α, 20β-diol Disulfateの3N塩酸煮沸による分解について : ステロイドの臨床分析(第26報)
- Mechanism of the D-Homoannulation of Pregnanediol Disulfate in Refluxing 3N Hydrochloric Acid
- Confirmation of the Involvement of C_-Carbonium Cation during the Hot Acid Hydrolysis of Pregnanediol Disulfate (Clinical Analysis on Steroids. XXIII
- Isolation and Structural Elucidation of the Degradation Products of Pregnanediol Disulfate obtained by Hot Acid Hydrolysis (Clinical Analysis on Steroids. XXI)
- HYDROLYSIS OF PREGNANEDIOL SULFATES IN BOILING HYDROCHLORIC ACID AND MECHANISM OF THE REARRANGEMENT REACTION FORMING Δ^-STEROID AS THE MAIN PRODUCT
- ステロイドの臨床分析(第16報)プレグナンジオール硫酸抱合体の合成
- On the Acid-Catalyzed D-Homoannulation of Pregnanetriol 20-Sulfate and Its C-20 Isomeric Sulfate
- ステロイドの臨床分析(第14報)2-ヒドロキシエストラジオール17β抱合体の合成
- Field Measurement on the Behavior of Low Rise Air-Supported Structure due to a Natural Wind
- Stable expression of CYP3A4 and CYP3A7, adult and fetal-specific forms of cytochrome P450 in human liver, in CHL cells and its application to toxicological testing.
- 「分析化学緑陰セミナー」にかかわって
- ステロイドの臨床分析(第18報)6,17-Dioxo-catechol Estrogenおよびその関連化合物の合成
- Studies on the Interactions between Drugs and Estrogen. III. Inhibitory Effects of 29 Drugs Reported to Induce Gynecomastia on the Glucuronidation of Estradiol(Miscellaneous)
- Studies on the Interactions between Drug and Estrogen. II. On the Inhibitory Effect of 29 Drugs Reported to Induce Gynecomastia on the Oxidation of Estradiol at C-2 or C-17
- High-Performance Liquid Chromatographic Separation of Potential Hydroxylated Metabolites of Estradiol 17-Sulfate by Female Rat Liver Microsomes
- Reaction of Adenine with 6-Hydroxyestrogen 6-Sulfates : Model Compounds to Demonstrate Carcinogenesis by Estrogen
- Evidence of Direct Conversion of Testosterone Sulfate to Estradiol 17-Sulfate by Human Placental Microsomes
- Chemical Evaluation of Betula Species in Japan. IV. Constituents of Betula davurica
- Chemical Evaluation of Betula Species in Japan. II. Constituents of Betula platyphylla var. japonica
- Chemical Evaluation of Betula Species in Japan. VI. Constituents of Betula schmidtii
- Chemical Evaluation of Betula Species in Japan. V. Constituents of Betula ovalifolia
- Chemical Evaluation of Betula Species in Japan. III. Constiutents of Betula maximowicziana
- TISSUE DISTRIBUTION OF ESTRADIOL 17-SULFATE 2- AND 4-HYDROXYLATION ENZYMES IN THE RAT
- STUDIES ON THE METABOLISM OF CONJUGATED CATECHOL ESTROGENS IN RATS
- Serum 2-Hydroxyestradiol 17-Sulphate in Pregnancy
- STUDIES ON NOVEL ANTIULCEROUS COMPOUNDS HAVING CYTOPROTECTIVE EFFECTS
- STUDIES ON METHODOLOGY OF FINDING THE ANTI-ALLERGIC AGENT WITH THE GUIDANCE OF ANTI-HYALURONIDASE ACTIVITY
- ACTIVATION OF HYALURONIDASE BY ANTITUMOR PLATINUM COMPLEX AND INHIBITION OF THE ACTIVATED ENZYME BY VARIOUS DRUGS
- HIGH SUSCEPTIBILITY TO AFLATOXIN B_1 AND BENZO[A]PYRENE OF BALB3T3 A31-1-1 CELLS EXPRESSING MONKEY CYP1A1
- EVIDENCE OF THE DIRECTIVE EFFECT OF 17β-CONJUGATE GROUP ON THE ENZYMATIC O-METHYLATION OF CATECHOL ESTROGEN
- IMMUNOCYTOCHEMICAL LOCALIZATION OF CATECHOL ESTROGENS IN THE RAT PITUITARY GLAND. : II.MEDIAN EMINENCE
- AN INDUCTION EFFECT OF PHENOBARBITAL ON RAT LIVER MICROSOMAL 4-HYDROXYLATION OF ESTRADIOL 17-SULFATE
- STUDIES ON THE METABOLISM OF ESTROGEN CONJUGATES BY HIGH-PERFORMANCE LIQUID CHROMATOGRAPHY
- INDUCTION OF LIVER MICROSOMAL 2-HYDROXYLATION OF ESTRADIOL 17-SULFATE BY PHENOBARBITAL IN MALE RAT
- ESTRADIOL 17β-SULFATE AS A SUBSTRATE FOR 2-HYDROXYLATION ENZYME OF RAT LIVER MICROSOMES (CLINICAL ANALYSIS ON STEROIDS. XX)
- THE EFFECT OF HYDROGEN ION CONCENTRATION ON ENZYMATIC O-METHYLATION OF CATECHOL ESTROGENS (CLINICAL ANALYSIS ON STEROIDS. XI)
- IMMUNOCYTOCHEMICAL LOCALIZATION OF CATECHOLESTROGEN IN THE RAT LIVER AFTER USING VARIOUS FIXATIVES
- MODULATION OF HYALURONIDASE ACTIVITY BY METAL SALTS AND DRUGS : THE CORRELATION WITH HISTAMINE SECRETION REACTION
- Quantitative Analysis of 17β-Estradiol in River Water by Fluorometric Enzyme Immunoassay Using Biotinylated Estradiol
- P-0835 CYP1B1によるエチニルエストラジオールの代謝(一般演題 ポスター発表,薬物病態(基礎),Enjoy Pharmacists' Lifestyles)
- Sepamtion and Estimation of Guaiacol Estrogens by High Performance Liquid Chmmatography