THE LONG-TERM EFFECTS OF THE RODENTICIDE, BRODIFACOUM, ON BLOOD-COAGULATION AND VITAMIN-K METABOLISM IN RATS

被引：39

作者：

MOSTERD, JJ ^{[1
]}

THIJSSEN, HHW ^{[1
]}

机构：

[1] STATE UNIV LIMBURG,DEPT PHARMACOL,6200 MD MAASTRICHT,NETHERLANDS

来源：

BRITISH JOURNAL OF PHARMACOLOGY | 1991年 / 104卷 / 02期

关键词：

ANTICOAGULATION; BINDING SITE; BRODIFACOUM; VITAMIN-K CYCLE; VITAMIN-K EPOXIDE REDUCTASE; WARFARIN;

D O I：

10.1111/j.1476-5381.1991.tb12463.x

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

1 The long-term (30 days) effects of a single dose of brodifacoum (0.2 mg kg-1, orally) on blood clotting activity and on liver parameters of the vitamin K cycle were investigated in rats. Maximal effect on blood clotting activity was seen on day one. On day seven blood clotting activity had returned to normal. 2 Liver microsomal vitamin KO reductase activity was maximally suppressed (10% of control activity) on day one, steadily recovered to about 40% on day 15 to remain at that level. The same time course was seen for the number of microsomal warfarin binding sites. 3 The persistent inhibition of the vitamin K cycle was also verified in vivo; following vitamin K administration (10 mg kg-1, i.v.) on day 30, the brodifacoum-treated rats accumulated vitamin KO in the liver. 4 Although clotting factor synthesis was normal, brodifacoum-treated rats were highly sensitive to warfarin. 5 Brodifacoum rapidly accumulated in the liver until the saturation of the microsomal binding site. Brodifacoum binding to the target prevented its elimination from the liver; liver content on day 30 was not different from day 7. 6 The results show (1) an over capacity for the hepatocellular vitamin K cycle, (2) a dissociation of the vitamin K epoxidation and the vitamin K-dependent carboxylation, (3) the 'superwarfarin' rodenticides to be extremely persistent due to their binding to the target.

引用

页码：531 / 535

页数：5

共 26 条

[11]

GREEFF MC, 1987, LANCET, V2, P1269

[12]

GRINNELL BW, 1990, BLOOD, V76, P2546

[13] MECHANISM OF COUMARIN ACTION - SENSITIVITY OF VITAMIN-K METABOLIZING ENZYMES OF NORMAL AND WARFARIN-RESISTANT RAT-LIVER [J].

HILDEBRANDT, EF ;

SUTTIE, JW .

BIOCHEMISTRY, 1982, 21 (10) :2406-2411

[14] THE FATE OF THE RODENTICIDE FLOCOUMAFEN IN THE RAT - RETENTION AND ELIMINATION OF A SINGLE ORAL DOSE [J].

HUCKLE, KR ;

HUTSON, DH ;

LOGAN, CJ ;

MORRISON, BJ ;

WARBURTON, PA .

PESTICIDE SCIENCE, 1989, 25 (03) :297-312

[15] A COMPARATIVE-STUDY OF THE EFFECTS OF WARFARIN AND BRODIFACOUM ON THE RELATIONSHIP BETWEEN VITAMIN-K1 METABOLISM AND CLOTTING FACTOR ACTIVITY IN WARFARIN-SUSCEPTIBLE AND WARFARIN-RESISTANT RATS [J].

LECK, JB ;

PARK, BK .

BIOCHEMICAL PHARMACOLOGY, 1981, 30 (02) :123-128

[16] ANTIBIOTIC-ASSOCIATED HYPOPROTHROMBINEMIA [J].

LIPSKY, JJ .

JOURNAL OF ANTIMICROBIAL CHEMOTHERAPY, 1988, 21 (03) :281-300

[17] THE FUNCTION AND METABOLISM OF VITAMIN-K [J].

OLSON, RE .

ANNUAL REVIEW OF NUTRITION, 1984, 4 :281-337

[18] ABNORMAL VITAMIN-K METABOLISM IN THE PRESENCE OF NORMAL CLOTTING FACTOR ACTIVITY IN FACTORY-WORKERS EXPOSED TO 4-HYDROXYCOUMARINS [J].

PARK, BK ;

CHOONARA, IA ;

HAYNES, BP ;

BRECKENRIDGE, AM ;

MALIA, RG ;

PRESTON, FE .

BRITISH JOURNAL OF CLINICAL PHARMACOLOGY, 1986, 21 (03) :289-293

[19]

SACHS L, 1984, ANGEWANDTE STATISTIK, P381

[20] RECENT ADVANCES IN HEPATIC VITAMIN-K METABOLISM AND FUNCTION [J].

SUTTIE, JW .

HEPATOLOGY, 1987, 7 (02) :367-376

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