HEPATOPROTECTIVE MECHANISM OF SILYMARIN - NO EVIDENCE FOR INVOLVEMENT OF CYTOCHROME-P450 2E1

被引：60

作者：

MIGUEZ, MP

ANUNDI, I

SAINZPARDO, LA

LINDROS, KO

机构：

[1] ALKO LTD, BIOMED RES CTR, SF-00101 HELSINKI, FINLAND

[2] UNIV EXTREMADURA, FAC VET, PHARMACOL & TOXICOL UNIT, CACERES, SPAIN

来源：

CHEMICO-BIOLOGICAL INTERACTIONS | 1994年 / 91卷 / 01期

关键词：

ALCOHOL; FLAVONOID ANTIOXIDANT; HEPATOPROTECTIVE MECHANISM; LIVER CYTOCHROME P450 2E1; SILYMARIN;

D O I：

10.1016/0009-2797(94)90006-X

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：

The involvement of the alcohol-inducible cytochrome P450 2E1 in the hepatoprotective mechanism of the plant flavonoid extract silymarin, and its main active component silybin, was investigated in isolated hepatocytes. Allyl alcohol toxicity, associated lipid peroxidation and GSH depletion was efficiently counteracted by silymarin (0.01-0.5 mM), and at higher concentrations by silybin. Cell damage by I-butyl hydroperoxide was also prevented by silymarin and silybin, but less efficiently. However, the covalent binding of the acetaminophen intermediate, formed via P450 2E1, was unaffected by addition of the flavonoids. Silybin did not influence microsomal 2E1-catalyzed demethylation of N-nitrosodimethylamine. Neither did demethylation of N-nitrosodimethylamine or aminopyrine by isolated microsomes affect the in vivo administration of silybin. Addition of silymarin or silybin to primary cultures of isolated hepatocytes did not prevent cell damage induced by exposure to the P450 2E1 substrate CCl4. In contrast, the mere presence of low concentrations (25-50 mu M) of these compounds was found to inhibit cell attachment to the matrix and eventually resulted in cell damage. We conclude that contrary to earlier reports we found no evidence for an interaction of silymarin or silybin with cytochrome P450 2E1. This suggests that the antioxidant and free radical scavenging properties may account for most of the therapeutic effect of these compounds. The untoward effect of silymarin on cultured cells may have consequences when considering long-term prescription of this therapeutic agent.

引用

页码：51 / 63

页数：13

共 32 条

[1] ALBANO E, 1985, MOL PHARMACOL, V28, P306
[2] ZONATION OF ACETAMINOPHEN METABOLISM AND CYTOCHROME-P450 2E1-MEDIATED TOXICITY STUDIED IN ISOLATED PERIPORTAL AND PERIVENOUS HEPATOCYTES
ANUNDI, I
LAHTEENMAKI, T
RUNDGREN, M
MOLDEUS, P
LINDROS, KO
[J]. BIOCHEMICAL PHARMACOLOGY, 1993, 45 (06) : 1251 - 1259
[3] ANUNDI I, 1992, Pharmacology and Toxicology, V70, P453
[4] INHIBITORY ACTION OF SILYMARIN OF LIPID PEROXIDE FORMATION IN RAT-LIVER MITOCHONDRIA AND MICROSOMES
BINDOLI, A
CAVALLINI, L
SILIPRANDI, N
[J]. BIOCHEMICAL PHARMACOLOGY, 1977, 26 (24) : 2405 - 2409
[5] FLUOROMETRIC ASSAY OF PROTEINS IN NANOGRAM RANGE
BOHLEN, P
STEIN, S
DAIRMAN, W
UDENFRIEND, S
[J]. ARCHIVES OF BIOCHEMISTRY AND BIOPHYSICS, 1973, 155 (01) : 213 - 220
[6] Campos R, 1988, Prog Clin Biol Res, V280, P375
[7] SILYBIN DIHEMISUCCINATE PROTECTS AGAINST GLUTATHIONE DEPLETION AND LIPID-PEROXIDATION INDUCED BY ACETAMINOPHEN ON RAT-LIVER
CAMPOS, R
GARRIDO, A
GUERRA, R
VALENZUELA, A
[J]. PLANTA MEDICA, 1989, (05) : 417 - 419
[8] LIPID-PEROXIDATION AND IRREVERSIBLE DAMAGE IN THE RAT HEPATOCYTE MODEL - PROTECTION BY THE SILYBIN PHOSPHOLIPID COMPLEX IDB-1016
CARINI, R
COMOGLIO, A
ALBANO, E
POLI, G
[J]. BIOCHEMICAL PHARMACOLOGY, 1992, 43 (10) : 2111 - 2115
[9] N-ACETYL-PARA-BENZOQUINONE IMINE - A CYTOCHROME-P-450-MEDIATED OXIDATION-PRODUCT OF ACETAMINOPHEN
DAHLIN, DC
MIWA, GT
LU, AYH
NELSON, SD
[J]. PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA-BIOLOGICAL SCIENCES, 1984, 81 (05): : 1327 - 1331
[10] RANDOMIZED CONTROLLED TRIAL OF SILYMARIN TREATMENT IN PATIENTS WITH CIRRHOSIS OF THE LIVER
FERENCI, P
DRAGOSICS, B
DITTRICH, H
FRANK, H
BENDA, L
LOCHS, H
MERYN, S
BASE, W
SCHNEIDER, B
[J]. JOURNAL OF HEPATOLOGY, 1989, 9 (01) : 105 - 113

← 1 2 3 4 →