Microsomal epoxide hydrolase of rat liver is a subunit of the anti-oestrogen-binding site

被引:28
|
作者
Mésange, F
Sebbar, M
Kedjouar, B
Capdevielle, J
Guillemot, JC
Ferrara, P
Bayard, F
Delarue, F
Faye, JC [1 ]
Poirot, M
机构
[1] CHU Rangueil, Inst Louis Bugnard, INSERM U397, F-31403 Toulouse 4, France
[2] Sanofi Elf Biorech, Lab Biochim Prot, F-31676 Labege, France
来源
BIOCHEMICAL JOURNAL | 1998年 / 334卷
关键词
D O I
10.1042/bj3340107
中图分类号
Q5 [生物化学]; Q7 [分子生物学];
学科分类号
071010 ; 081704 ;
摘要
A tritiated photoaffinity labelling analogue of tamoxifen, [(2-azido-4-benzyl)-phenoxy]-N-ethylmorpholine (azido-MBPE), was used to identify the anti-oestrogen-binding site (AEBS) in rat liver tissue [Poirot, Chailleux, Fargin, Bayard and Faye (1990) J, Biol, Chem, 265, 17039-17043]. UV irradiation of rat liver microsomal proteins incubated with tritiated azido-MBPE led to the characterization of two photolabelled proteins of molecular masses 40 and 50 kDa. The amino acid sequences of proteolytic products from the 50 kDa protein were identical with those from rat microsomal epoxide hydrolase (mEH). Treatment of hepatocytes with anti-sense mRNA directed against mEH abolished AEBS in these cells. In addition we found that tamoxifen and N-morpholino-2-[4-(phenylmethyl)phenoxy] ethanamine, a selective ligand of AEBS, were potent inhibitors of the catalytic hydration of styrene oxide by mEH. However, functional overexpression of the human mEH did not significantly modify the binding capacity of [H-3]tamoxifen. Taken together, these results suggest that the 50 kDa protein, mEH, is necessary but not sufficient to reconstitute AEBS.
引用
收藏
页码:107 / 112
页数:6
相关论文
共 50 条
  • [1] ASSESSMENT OF RAT-LIVER MICROSOMAL EPOXIDE HYDROLASE AS A MARKER OF HEPATOCARCINOGENESIS
    KIZER, DE
    CLOUSE, JA
    RINGER, DP
    HANSONPAINTON, O
    VAZ, AD
    PALAKODETY, RB
    GRIFFIN, MJ
    BIOCHEMICAL PHARMACOLOGY, 1985, 34 (10) : 1795 - 1800
  • [2] MICROSOMAL EPOXIDE HYDROLASE IN DIFFERENT RAT STRAINS
    OESCH, F
    ZIMMER, A
    GLATT, HR
    BIOCHEMICAL PHARMACOLOGY, 1983, 32 (11) : 1783 - 1788
  • [3] ENDOGENOUS PHOSPHORYLATION OF PHOSPHATIDYLINOSITOL BOUND TO RAT-LIVER MICROSOMAL EPOXIDE HYDROLASE
    PALAKODETY, RB
    FOX, OF
    WONG, NS
    HANSONPAINTON, O
    JACKSON, KW
    GRIFFIN, MJ
    FEDERATION PROCEEDINGS, 1983, 42 (07) : 1771 - 1771
  • [4] EXPRESSION OF RAT MICROSOMAL EPOXIDE HYDROLASE GENE DURING LIVER CHEMICAL CARCINOGENESIS
    KONDO, S
    CARR, BI
    TAKAGI, K
    HUANG, TH
    CHOU, YM
    YOKOYAMA, K
    ITAKURA, K
    CANCER RESEARCH, 1990, 50 (19) : 6222 - 6228
  • [5] A NEW ENZYME-IMMUNOASSAY OF MICROSOMAL RAT-LIVER EPOXIDE HYDROLASE
    ZHIRI, A
    MULLER, J
    FOURNEL, S
    MAGDALOU, J
    WELLMANBEDNAWSKA, M
    SIEST, G
    ANALYTICAL BIOCHEMISTRY, 1987, 163 (02) : 298 - 302
  • [6] PURIFICATION AND CHARACTERIZATION OF DOG LIVER MICROSOMAL EPOXIDE HYDROLASE
    ARIYOSHI, N
    TANAKA, M
    ISHII, Y
    OGURI, K
    JOURNAL OF BIOCHEMISTRY, 1994, 115 (05): : 985 - 990
  • [7] EXPRESSION OF RAT MICROSOMAL EPOXIDE HYDROLASE DURING PREGNANCY
    KIM, SG
    BIOCHEMICAL PHARMACOLOGY, 1995, 50 (10) : 1593 - 1597
  • [8] Induction of Microsomal Epoxide Hydrolase by Tienilic Acid in the Rat
    Sellman, R.
    Parkki, M. G.
    JOURNAL OF APPLIED TOXICOLOGY, 1983, 3 (05) : 245 - 248
  • [9] HUMAN-LIVER MICROSOMAL EPOXIDE HYDROLASE (H-EH) - IMMUNOCHEMICAL AND STRUCTURAL-PROPERTIES COMPARED WITH RAT-LIVER MICROSOMAL EPOXIDE HYDROLASE (R-EH)
    THOMAS, PE
    VONBAHR, C
    GLAUMANN, H
    JERINA, DM
    LEVIN, W
    FEDERATION PROCEEDINGS, 1981, 40 (06) : 1836 - 1836
  • [10] Enhanced expression of rat hepatic microsomal epoxide hydrolase by methylthiazole in conjunction with liver injury
    Cho, MK
    Kim, SG
    TOXICOLOGY, 2000, 146 (2-3) : 111 - 122
12345