POTENTIATION OF BROMOBENZENE-INDUCED PNEUMOTOXICITY BY PHENOBARBITAL AS DETERMINED BY BRONCHOALVEOLAR LAVAGE FLUID ANALYSIS

被引：5

作者：

DAY, BJ ^{[1
]}

DENICOLA, DB ^{[1
]}

CARLSON, GP ^{[1
]}

机构：

[1] PURDUE UNIV,SCH VET MED,DEPT PATHOBIOL,W LAFAYETTE,IN 47907

来源：

DRUG AND CHEMICAL TOXICOLOGY | 1992年 / 15卷 / 01期

关键词：

D O I：

10.3109/01480549209035171

中图分类号：

O6 [化学];

学科分类号：

0703 ;

摘要：

Bromobenzene produces pulmonary, renal and hepatic damage in the rat. Phenobarbital potentiates bromobenzene-induced hepatotoxicity. Studies were initiated to determine if phenobarbital potentiates the pulmonary damage produced by bromobenzene. In a dose ranging study, adult male rats were treated daily for 4 days with phenobarbital (80 mg/kg, ip) and on the fifth day were dosed with 0, 2, 3, or 4 mmoles/kg, ip, bromobenzene. In a larger study phenobarbital was given for 4 days (80 mg/kg, ip), and bromobenzene (3.3 mmoles/kg, ip) was given on the fifth day. Pulmonary damage was assessed 24 hours later in the first study and 12 hours later in the second study by bronchoalveolar lavage fluid analysis (BALF), microsomal mixed function oxidase measurements and histopathological evaluations. BALF biochemical markers employed were gamma-glutamyl transpeptidase (GGT), lactate dehydrogenase (LDH) and total protein. Phenobarbital treatment greatly enhanced bromobenzene-induced GGT and LDH release into the lavage fluid in a dose-dependent manner. Phenobarbital treatment increased microsomal 7-O-dealkylation of both ethoxy- and pentoxyresorufin in the liver without affecting these activities in the lung. Bromobenzene treatment decreased the hepatic microsomal dealkylation of pentoxyresorufin in a dose-dependent manner. Since known rat pulmonary P450 isozymes have been reported to be insensitive to phenobarbital induction, it may be that the toxicity is due to transport of a reactive metabolite(s) formed in the liver to the lung or bromobenzene is activated by some other pulmonary P450 isozyme responsive to phenobarbital.

引用

页码：33 / 51

页数：19

共 25 条

[1]

ALVARES AP, 1987, CURRENT TOPICS PULMO, V2, P136

[2]

BOYD JW, 1982, VET CLIN PATH, V12, P9

[3] EVIDENCE FOR CLARA CELL AS A SITE OF CYTOCHROME P450-DEPENDENT MIXED-FUNCTION OXIDASE ACTIVITY IN LUNG [J].

BOYD, MR .

NATURE, 1977, 269 (5630) :713-715

[4]

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

[5] POSSIBLE MECHANISM OF LIVER NECROSIS CAUSED BY AROMATIC ORGANIC COMPOUNDS [J].

BRODIE, BB ;

REID, WD ;

CHO, AK ;

SIPES, G ;

KRISHNA, G ;

GILLETTE, JR .

PROCEEDINGS OF THE NATIONAL ACADEMY OF SCIENCES OF THE UNITED STATES OF AMERICA, 1971, 68 (01) :160-&

[6] ETHOXYPHENOXAZONES, PENTOXYPHENOXAZONES, AND BENZYLOXYPHENOXAZONES AND HOMOLOGS - A SERIES OF SUBSTRATES TO DISTINGUISH BETWEEN DIFFERENT INDUCED CYTOCHROMES-P-450 [J].

BURKE, MD ;

THOMPSON, S ;

ELCOMBE, CR ;

HALPERT, J ;

HAAPARANTA, T ;

MAYER, RT .

BIOCHEMICAL PHARMACOLOGY, 1985, 34 (18) :3337-3345

[7] SPECIES-DIFFERENCES IN SHORT-TERM TOXICITY FROM INHALATION EXPOSURE TO BROMOBENZENE [J].

DAHL, JE ;

BECHER, R ;

AARSTAD, K ;

NILSEN, OG ;

DYBING, E .

ARCHIVES OF TOXICOLOGY, 1990, 64 (05) :370-376

[8] GAMMA-GLUTAMYL-TRANSPEPTIDASE IN RAT BRONCHOALVEOLAR LAVAGE FLUID AS A PROBE OF 4-IPOMEANOL AND ALPHA-NAPHTHYLTHIOUREA-INDUCED PNEUMOTOXICITY [J].

DAY, BJ ;

CARLSON, GP ;

DENICOLA, DB .

JOURNAL OF PHARMACOLOGICAL METHODS, 1990, 24 (01) :1-8

[9] EARLY DAMAGE INDICATORS IN THE LUNG .5. BIOCHEMICAL AND CYTOLOGICAL RESPONSE TO NO2 INHALATION [J].

DENICOLA, DB ;

REBAR, AH ;

HENDERSON, RF .

TOXICOLOGY AND APPLIED PHARMACOLOGY, 1981, 60 (02) :301-312

[10] XENOBIOTIC METABOLISM BY ISOLATED PULMONARY CELLS [J].

DEVEREUX, TR ;

DOMIN, BA ;

PHILPOT, RM .

PHARMACOLOGY & THERAPEUTICS, 1989, 41 (1-2) :243-256

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