4-(4-NITROBENZYL)PYRIDINE TESTS FOR ALKYLATING-AGENTS FOLLOWING CHEMICAL OXIDATIVE ACTIVATION

被引：13

作者：

THOMAS, JJ ^{[1
]}

KIM, JH ^{[1
]}

MAURO, DM ^{[1
]}

机构：

[1] UNIV MICHIGAN,SCH PUBL HLTH,DEPT ENVIRONM & IND HLTH,ENVIRONM CHEM PROGRAM,ANN ARBOR,MI 48109

来源：

ARCHIVES OF ENVIRONMENTAL CONTAMINATION AND TOXICOLOGY | 1992年 / 22卷 / 02期

关键词：

D O I：

10.1007/BF00213289

中图分类号：

X [环境科学、安全科学];

学科分类号：

08 ; 0830 ;

摘要：

A chemical activation system (CAS) designed to mimic the mammalian mixed-function oxidase enzymes was found to activate target compounds to reactive electrophiles. Activated compounds were assayed by reaction with 4-(4-nitrobenzyl)pyridine (NBP). A model nucleophile of 7-alkylguanine of nucleic acids, NBP produces a violet color following alkylation. Twenty compounds from several chemical classes were tested. The test generally gave positive and negative responses where expected. Two compounds, trichloroethylene and diethylnitrosamine, exhibited a linear Beer's law relationship in the concentration range tested. A high degree of linear correlation (r > 0.97) was obtained for these compounds. Other compounds showed varying degrees of linear correlation from high correlation (r = 0.94) to weak correlation (r = 0.44). The CAS-NBP assay results were compared to bacterial mutagenicity and animal carcinogenicity test results when information was available. A good correlation (r = 0.80) existed between direct alkylating activity and direct mutagenicity. Similar correlations existed between NBP alkylation following activation and mutagenicity following microsomal activation (r = 0.73). Also, different correlations were observed between carcinogenicity and NBP alkylation following activation (r = 0.69) and without activation (r = 0.38).

引用

页码：219 / 227

页数：9

共 39 条

[1] THE INVITRO UNSCHEDULED DNA-SYNTHESIS (UDS) ASSAY IN RAT PRIMARY HEPATOCYTES - EVALUATION OF 2-FUROIC ACID AND 7 DRUG CANDIDATES [J].

AARON, CS ;

HARBACH, PR ;

WISER, SK ;

GRZEGORCZYK, CR ;

SMITH, AL .

MUTATION RESEARCH, 1989, 223 (02) :163-169

[2] QUANTITATIVE-DETERMINATION OF CARCINOGENS AND MUTAGENS AS ALKYLATING-AGENTS FOLLOWING CHEMICAL ACTIVATION [J].

ARCHER, MC ;

ENG, VWS .

CHEMICO-BIOLOGICAL INTERACTIONS, 1981, 33 (2-3) :207-214

[3] A STUDY OF COMPARATIVE CHEMICAL AND BIOLOGICAL ACTIVITIES OF ALKYLATING AGENTS [J].

BARDOS, TJ ;

DATTAGUP.N ;

HEBBORN, P ;

TRIGGLE, DJ .

JOURNAL OF MEDICINAL CHEMISTRY, 1965, 8 (02) :167-&

[4] QUANTITATIVE COMPARISON OF CARCINOGENICITY, MUTAGENICITY AND ELECTROPHILICITY OF 10 DIRECT-ACTING ALKYLATING-AGENTS AND OF THE INITIAL O-6-7-ALKYLGUANINE RATIO IN DNA WITH CARCINOGENIC POTENCY IN RODENTS [J].

BARTSCH, H ;

TERRACINI, B ;

MALAVEILLE, C ;

TOMATIS, L ;

WAHRENDORF, J ;

BRUN, G ;

DODET, B .

MUTATION RESEARCH, 1983, 110 (02) :181-219

[5]

Bogaert M. D., 1981, TOXICOL LETT, V7, P311

[6] MUTAGENIC ACTIVITY OF 61 AGENTS AS DETERMINED BY THE MICRONUCLEUS, SALMONELLA, AND SPERM ABNORMALITY ASSAYS [J].

BRUCE, WR ;

HEDDLE, JA .

CANADIAN JOURNAL OF GENETICS AND CYTOLOGY, 1979, 21 (03) :319-333

[7] REVIEW OF EXPERIMENTAL CARCINOGENESIS BY COMPOUNDS RELATED TO VINYL-CHLORIDE [J].

CHU, KC ;

MILMAN, HA .

ENVIRONMENTAL HEALTH PERSPECTIVES, 1981, 41 (OCT) :211-220

[8] ACRYLAMIDE - ITS METABOLISM, DEVELOPMENTAL AND REPRODUCTIVE EFFECTS, GENOTOXICITY, AND CARCINOGENICITY [J].

DEARFIELD, KL ;

ABERNATHY, CO ;

OTTLEY, MS ;

BRANTNER, JH ;

HAYES, PF .

MUTATION RESEARCH, 1988, 195 (01) :45-77

[9] MUTAGENIC POTENTIAL OF ALLYL AND ALLYLIC COMPOUNDS - STRUCTURE-ACTIVITY RELATIONSHIP AS DETERMINED BY ALKYLATING AND DIRECT INVITRO MUTAGENIC PROPERTIES [J].

EDER, E ;

NEUDECKER, T ;

LUTZ, D ;

HENSCHLER, D .

BIOCHEMICAL PHARMACOLOGY, 1980, 29 (07) :993-998

[10] GENETIC TOXICITY OF SOME IMPORTANT EPOXIDES [J].

EHRENBERG, L ;

HUSSAIN, S .

MUTATION RESEARCH, 1981, 86 (01) :1-113

← 1 2 3 4 →