REDUCED ACTIVITIES OF KEY ENZYMES OF GLUCONEOGENESIS AS POSSIBLE CAUSE OF ACUTE TOXICITY OF 2,3,7,8-TETRACHLORODIBENZO-PARA-DIOXIN (TCDD) IN RATS

被引：62

作者：

WEBER, LWD

LEBOFSKY, M

STAHL, BU

GORSKI, JR

MUZI, G

ROZMAN, K

机构：

[1] GESELL STRAHLEN & UMWELTFORSCH MBH,INST TOXIKOL,ENVIRONM TOXICOL SECT,INGOLSTADTER LANDSTR 1,W-8042 NEUHERBERG,GERMANY

[2] UNIV KANSAS,MED CTR,DEPT PHARMACOL TOXICOL & THERAPEUT,KANSAS CITY,KS 66103

来源：

TOXICOLOGY | 1991年 / 66卷 / 02期

关键词：

2,3,7,8-TETRACHLORODIBENZO-PARA-DIOXIN; GLUCONEOGENESIS; TIME COURSE; PHOSPHOENOLPYRUVATE CARBOXYKINASE; GLUCOSE-6-PHOSPHATASE; ACUTE TOXICITY;

D O I：

10.1016/0300-483X(91)90214-L

中图分类号：

R9 [药学];

学科分类号：

1007 ;

摘要：

Male Sprague-Dawley rats (350-375 g) were injected i.p. with TCDD (25 [sublethal dose] and 125-mu-g/kg [lethal dose], respectively, in corn oil/acetone), or vehicle only; vehicle-treated animals were pair-fed to their TCDD-treated counterparts. 1, 2, 4, 8, 16, and 32 days (28 days for lethal dose) thereafter, animals were sacrificed and activities of two key enzymes of gluconeogenesis determined in livers of rats. In livers of pair-fed rats both enzyme activities were little affected. In the livers of TCDD-treated animals the activity of phosphoenolpyruvate carboxykinase (PEPCK, EC 4.1.1.32) decreased rapidly, exhibiting significant losses by the 2nd day after treatment. Time course and extent of loss of PEPCK activity (about 50%) were similar after either dose. The activity of glucose-6-phosphatase (G-6-Pase, EC 3.1.3.9) decreased more slowly as a result of TCDD treatment; statistically significant losses were observed by 4 or 8 days after the lethal and sublethal dose, respectively. These results confirm the hypothesis that reduced in vivo rates of gluconeogenesis in TCDD-treated rats are due to decreased activities of gluconeogenic enzymes. In an additional set of experiments, rats were treated with 125-mu-g/kg TCDD, 25-mu-g/kg TCDD, or with vehicle alone. The 25-mu-g/kg or vehicle-treated rats were then pair-fed to rats dosed with 125-mu-g/kg of TCDD. Mean time to death and body weight loss at the time of death were essentially identical in all groups, lending additional support to the hypothesis that reduced feed intake is the major cause of TCDD-induced death in male Sprague-Dawley rats. Both appetite suppression and reduced total PEPCK activity in whole livers occurred in the same dose-ranges of TCDD, suggesting the possibility of a cause-effect relationship.

引用

页码：133 / 144

页数：12

共 26 条

[1] TISSUE DISTRIBUTION, EXCRETION AND BIOLOGICAL EFFECTS OF [C-14]TETRACHLORODIBENZO-PARA-DIOXIN IN RATS [J].

ALLEN, JR ;

VANMILLER, JP ;

NORBACK, DH .

FOOD AND COSMETICS TOXICOLOGY, 1975, 13 (05) :501-&

[2]

BAGINSKY ES, 1974, METHOD ENZYMAT AN, V1, P876

[3]

BRADFORD MM, 1976, ANAL BIOCHEM, V72, P248, DOI 10.1016/0003-2697(76)90527-3

[4]

BUTLER PC, 1989, ENDOCRIN METAB CLIN, V18, P1

[5] RELATIONSHIP OF THE WASTING SYNDROME TO LETHALITY IN RATS TREATED WITH 2,3,7,8-TETRACHLORODIBENZO-PARA-DIOXIN [J].

CHRISTIAN, BJ ;

INHORN, SL ;

PETERSON, RE .

TOXICOLOGY AND APPLIED PHARMACOLOGY, 1986, 82 (02) :239-255

[6] INTERMEDIARY METABOLISM OF THE MATURE RAT FOLLOWING 2,3,7,8-TETRACHLORODIBENZO-PARA-DIOXIN TREATMENT [J].

CHRISTIAN, BJ ;

MENAHAN, LA ;

PETERSON, RE .

TOXICOLOGY AND APPLIED PHARMACOLOGY, 1986, 83 (02) :360-378

[7] GLUCONEOGENESIS [J].

EXTON, JH .

METABOLISM-CLINICAL AND EXPERIMENTAL, 1972, 21 (10) :945-+

[8] DOSE-RESPONSE AND TIME COURSE OF HYPOTHYROXINEMIA AND HYPOINSULINEMIA AND CHARACTERIZATION OF INSULIN HYPERSENSITIVITY IN 2,3,7,8-TETRACHLORODIBENZO-PARA-DIOXIN (TCDD) TREATED RATS [J].

GORSKI, JR ;

ROZMAN, K .

TOXICOLOGY, 1987, 44 (03) :297-307

[9] ELEVATED PLASMA-CORTICOSTERONE LEVELS AND HISTOPATHOLOGY OF THE ADRENALS AND THYMUSES IN 2,3,7,8-TETRACHLORODIBENZO-PARA-DIOXIN-TREATED RATS [J].

GORSKI, JR ;

MUZI, G ;

WEBER, LW ;

PEREIRA, DW ;

IATROPOULOS, MJ ;

ROZMAN, K .

TOXICOLOGY, 1988, 53 (01) :19-32

[10] SOME ENDOCRINE AND MORPHOLOGICAL ASPECTS OF THE ACUTE TOXICITY OF 2,3,7,8-TETRACHLORODIBENZO-P-DIOXIN (TCDD) [J].

GORSKI, JR ;

MUZI, G ;

WEBER, LWD ;

PEREIRA, DW ;

ARCEO, RJ ;

IATROPOULOS, MJ ;

ROZMAN, K .

TOXICOLOGIC PATHOLOGY, 1988, 16 (03) :313-320

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