CORRELATION OF CARCINOGENIC POTENCY WITH MOUSE-SKIN P-32 POSTLABELING AND MUTA-RMOUSE LAC Z- MUTATION DATA FOR DMBA AND ITS K-REGION SULFUR ISOSTERE - COMPARISON WITH ACTIVITIES OBSERVED IN STANDARD GENOTOXICITY ASSAYS

被引：27

作者：

ASHBY, J

BRUSICK, D

MYHR, BC

JONES, NJ

PARRY, JM

NESNOW, S

PATON, D

TINWELL, H

ROSENKRANZ, HS

CURTI, S

GILMAN, D

CALLANDER, RD

机构：

[1] HAZLETON WASHINGTON INC,MOLEC & CELLULAR TOXICOL,VIENNA,VA 22182

[2] ENVIRONM HLTH RES & TESTING INC,RES TRIANGLE PK,NC 27709

[3] UNIV PITTSBURGH,GRAD SCH PUBL HLTH,PITTSBURGH,PA 15261

[4] UNIV COLL SWANSEA,SCH BIOL SCI,SWANSEA SA2 8PP,W GLAM,WALES

[5] US EPA,CARCINOGENESIS & METAB BRANCH,RES TRIANGLE PK,NC 27711

来源：

MUTATION RESEARCH | 1993年 / 292卷 / 01期

关键词：

CARCINOGENIC POTENCY; CORRELATION; MOUSE SKIN; P-32-POSTLABELING; LAC Z- MUTATION DATA; DMBA; 7,12-DIMETHYLBENZ[A]ANTHRACENE; S-DMBA; 6,11-DIMETHYLBENZO[B]NAPHTHO[2,3-D]THIOPHENE;

D O I：

10.1016/0165-1161(93)90005-K

中图分类号：

Q3 [遗传学];

学科分类号：

071007 ; 090102 ;

摘要：

The genotoxicities in vitro and in vivo of the mouse-skin carcinogen 7,12-dimethylbenz[a]anthracene (DMBA) have been compared with those of its weakly carcinogenic 4,5-sulphur analogue, 6,11-dimethyl-benzo[b]naphtho-[2,3-d]thiophene (S-DMBA). The only datasets that correlated with the relative carcinogenicity of these agents to the skin were those conducted using topically exposed mouse skin. Thus, both chemicals induced lacZ- mutations in the skin of lacZ+ transgenic mice, and both produced DNA adducts on mouse-skin DNA as assessed using the P-32-postlabeling technique. In each case, DMBA gave a stronger response than did S-DMBA. In contrast to these responses, only DMBA was active in the mouse bone-marrow micronucleus assay and in the C3H10T1/2 in vitro cell transformation assay. Both chemicals were mutagenic to Salmonella and of approximately equal potency. The molecular geometry of DMBA and S-DMBA are compared, and divergent CASE predictions of activity in the Salmonella assay and skin-painting bioassay are discussed. The importance of conducting predictive genotoxicity assays in systems close to those in which carcinogenicity is to be assessed is emphasized by these data.

引用

页码：25 / 40

页数：16

共 52 条

[21]

HARTWELL JL, 1951, SURVEY COOMPOUNDS WH

[22] AN APPLICATION OF ACRIDINE-ORANGE FLUORESCENT STAINING TO THE MICRONUCLEUS TEST [J].

HAYASHI, M ;

SOFUNI, T ;

ISHIDATE, M .

MUTATION RESEARCH, 1983, 120 (04) :241-247

[23] CELL-TRANSFORMATION BY CHEMICAL-AGENTS - A REVIEW AND ANALYSIS OF THE LITERATURE - A REPORT OF THE UNITED-STATES-ENVIRONMENTAL-PROTECTION-AGENCY GENE-TOX PROGRAM [J].

HEIDELBERGER, C ;

FREEMAN, AE ;

PIENTA, RJ ;

SIVAK, A ;

BERTRAM, JS ;

CASTO, BC ;

DUNKEL, VC ;

FRANCIS, MW ;

KAKUNAGA, T ;

LITTLE, JB ;

SCHECHTMAN, LM .

MUTATION RESEARCH, 1983, 114 (03) :283-385

[24]

HENNINGS H, 1981, CANCER RES, V41, P773

[25] REFINEMENT OF STRUCTURE OF 9 - 10-DIMETHYL-1 - 2-BENZANTHRACENE [J].

IBALL, J .

NATURE, 1964, 201 (492) :916-&

[26]

Jerina D.M., 1978, POLYCYCLIC HYDROCARB, V1, P173

[27] P-32 POSTLABELING ANALYSIS AND MICRONUCLEI INDUCTION IN PRIMARY CHINESE-HAMSTER LUNG-CELLS EXPOSED TO TOBACCO PARTICULATE MATTER [J].

JONES, NJ ;

KADHIM, MA ;

HOSKINS, PL ;

PARRY, JM ;

WATERS, R .

CARCINOGENESIS, 1991, 12 (08) :1507-1514

[28]

MILLER EC, 1961, CANCER RES, V21, P815

[29]

MILLER EC, 1966, PHARMACOL REV, V18, P805

[30]

MILLER JA, 1963, CANCER RES, V23, P229

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