INHIBITORY EFFECTS OF ANTIOXIDANTS ON N-BIS(2-HYDROXYPROPYL)NITROSAMINE-INDUCED LUNG CARCINOGENESIS IN RATS

被引：36

作者：

HASEGAWA, R ^{[1
]}

FURUKAWA, F ^{[1
]}

TOYODA, K ^{[1
]}

TAKAHASHI, M ^{[1
]}

HAYASHI, Y ^{[1
]}

HIROSE, M ^{[1
]}

ITO, N ^{[1
]}

机构：

[1] NATL INST HYG SCI, DIV PATHOL, SETAGAYA KU, TOKYO 158, JAPAN

来源：

JAPANESE JOURNAL OF CANCER RESEARCH | 1990年 / 81卷 / 09期

关键词：

Antioxidant; Lung tumorigenesis; nhibition; Rat;

D O I：

10.1111/j.1349-7006.1990.tb02660.x

中图分类号：

R73 [肿瘤学];

学科分类号：

100214 ;

摘要：

Potential second‐stage modifying effects of 8 antioxidants on lung tumorigenesis initiated by N‐bis(2‐hydroxypropyl)nitrosamine (DHPN) were examined in male F344 rats. After an initial 2‐week treatment with DHPN (0.1% in drinking water), rats were administered one of the antioxidants supplemented in the diet for 30 weeks. Although the incidences of lung adenomas were not affected, those of carcinomas were lowered by 2% butylated hydroxyanisole (BHA, 2 rats/20 rats), 1% butylated hydroxytoluene (BHT, 1/20), 0.8% ethoxyquin (EQ, 3/20) and 1%α‐tocopherol (α‐TP, 2/20) treatments as compared to the control level (9/20), while 5% sodium l‐ascorbate (SA), 0.8% catechol (CC), 0.8% resorcinol (RN), and 0.8% hydroquinone (HQ) did not exert any significant effect on incidence. Quantitative analysis of adenomas and carcinomas (numbers and areas of lesions per unit area of lung section) revealed obvious inhibitory effects of SA, CC, and RN as well as BHA, BHT, EQ, and α‐TP. Among the antioxidants, BHT exerted the strongest inhibitory activity. In contrast, DHPN‐induced thyroid tumorigenesis was significantly enhanced by BHT (14/20) and EQ (20/20) treatments (control=5/20). Thus the antioxidants showed opposite effects on lung and thyroid carcinogenesis in the rat. Copyright © 1990, Wiley Blackwell. All rights reserved

引用

页码：871 / 877

页数：7

共 37 条

[21]

MALKINSON AM, 1986, CANCER RES, V46, P1694

[22] ETHOXYQUIN ALONE INDUCES PRENEOPLASTIC CHANGES IN RAT-KIDNEY WHILE PREVENTING INDUCTION OF SUCH LESIONS IN LIVER BY AFLATOXIN-B1 [J].

MANSON, MM ;

GREEN, JA ;

DRIVER, HE .

CARCINOGENESIS, 1987, 8 (05) :723-728

[23]

MASUI T, 1986, JPN J CANCER RES, V77, P1083

[24]

NEWMARK HL, 1981, INHIBITION TUMOR IND, P127

[25]

RAWSON RW, 1981, INHIBITION TUMOR IND, P219

[26] ORGAN SPECIFIC MODIFYING POTENTIAL OF ETHINYL ESTRADIOL ON CARCINOGENESIS INITIATED WITH DIFFERENT CARCINOGENS [J].

SHIRAI, T ;

TSUDA, H ;

OGISO, T ;

HIROSE, M ;

ITO, N .

CARCINOGENESIS, 1987, 8 (01) :115-119

[27] MODIFICATION BY 5 ANTIOXIDANTS OF 1,2-DIMETHYLHYDRAZINE-INITIATED COLON CARCINOGENESIS IN F344 RATS [J].

SHIRAI, T ;

IKAWA, E ;

HIROSE, M ;

THAMAVIT, W ;

ITO, N .

CARCINOGENESIS, 1985, 6 (04) :637-639

[28]

SHIRAI T, 1984, JPN J CANCER RES, V75, P502

[29] MODIFICATION BY ALPHA-TOCOPHEROL, PROPYL GALLATE AND TERTIARY BUTYLHYDROQUINONE OF URINARY-BLADDER CARCINOGENESIS IN FISCHER 344 RATS PRETREATED WITH N-BUTYL-N-(4-HYDROXYBUTYL)NITROSAMINE [J].

TAMANO, S ;

FUKUSHIMA, S ;

SHIRAI, T ;

HIROSE, M ;

ITO, N .

CANCER LETTERS, 1987, 35 (01) :39-46

[30] MODIFYING EFFECTS OF BUTYLATED HYDROXYANISOLE, ETHOXYQUIN AND ACETAMINOPHEN ON INDUCTION OF NEOPLASTIC LESIONS IN RAT-LIVER AND KIDNEY INITIATED BY N-ETHYL-N-HYDROXYETHYLNITROSAMINE [J].

TSUDA, H ;

SAKATA, T ;

MASUI, T ;

IMAIDA, K ;

ITO, N .

CARCINOGENESIS, 1984, 5 (04) :525-531

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