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苯并[a]芘和3-甲基胆蒽的氟化衍生物在小鼠皮肤中的肿瘤起始活性及在大鼠乳腺中的致癌性。

Tumor-initiating activity in mouse skin and carcinogenicity in rat mammary gland of fluorinated derivatives of benzo[a]pyrene and 3-methylcholanthrene.

作者信息

Cavalieri E, Rogan E, Higginbotham S, Cremonesi P, Salmasi S

机构信息

Eppley Institute for Research in Cancer, Omaha, NE.

出版信息

J Cancer Res Clin Oncol. 1988;114(1):16-22. doi: 10.1007/BF00390480.

Abstract

Comparative studies of tumor-initiating activity in mouse skin and carcinogenicity in rat mammary gland were conducted with benzo[a]pyrene (BP) and 3-methylcholanthrene (MC) derivatives. SENCAR mice were initiated with BP, 6-fluorobenzo[a]pyrene (6-FBP), 6-methylBP, 7-FBP, 8-FBP, 9-FBP, 10-FBP, or 10-azaBP and promoted with tetradecanoyl phorbol acetate. The same compounds plus BP 7,8-dihydrodiol were tested by intramammillary injection in female Sprague-Dawley rats. Tumor-initiating activity in mice and/or carcinogenicity in rats were observed for BP, 6-methylBP, 6-, 7-, 8-, and 10-FBP, whereas 9-FBP was inactive in both experiments and 10-azaBP was only marginally active in the mammary gland. BP 7,8-dihydrodiol was carcinogenic in rat mammary gland, although it was less potent than BP. MC, 8-FMC, 10-FMC, and 3-methylcholanthrylene were also tested in Sprague-Dawley rats by intramammillary injection. All compounds were carcinogenic, with MC displaying the most potent activity. The less potent carcinogenic activity of BP 7,8-dihydrodiol in the mammary gland, compared with BP, and the moderate-to-weak tumor-initiating and/or carcinogenic activity of 7-, 8-, and 10-FBP suggest that the bay-region diol-epoxide pathway does not play a significant role in the activation of BP in these two target tissues. Similarly, the carcinogenic activity of 8-FMC and 10-FMC, in which the bay-region diol-epoxide pathway is blocked, suggests that this mechanism of activation is not important in the carcinogenicity of MC in rat mammary gland.

摘要

用苯并[a]芘(BP)和3-甲基胆蒽(MC)衍生物进行了小鼠皮肤肿瘤起始活性和大鼠乳腺致癌性的比较研究。用BP、6-氟苯并[a]芘(6-FBP)、6-甲基BP、7-FBP、8-FBP、9-FBP、10-FBP或10-氮杂BP对SENCAR小鼠进行启动,并用地塞米松十四烷酸酯进行促进。通过乳内注射在雌性Sprague-Dawley大鼠中测试相同的化合物加BP 7,8-二氢二醇。观察到BP、6-甲基BP、6-、7-、8-和10-FBP在小鼠中的肿瘤起始活性和/或在大鼠中的致癌性,而9-FBP在两个实验中均无活性,10-氮杂BP在乳腺中仅具有微弱活性。BP 7,8-二氢二醇在大鼠乳腺中具有致癌性,尽管其效力低于BP。还通过乳内注射在Sprague-Dawley大鼠中测试了MC、8-FMC、10-FMC和3-甲基胆蒽。所有化合物均具有致癌性,其中MC显示出最强的活性。与BP相比,BP 7,8-二氢二醇在乳腺中的致癌活性较低,以及7-、8-和10-FBP的中度至弱的肿瘤起始和/或致癌活性表明,湾区二醇环氧化物途径在这两个靶组织中BP的活化中不起重要作用。同样,8-FMC和10-FMC的致癌活性,其中湾区二醇环氧化物途径被阻断,表明这种活化机制在大鼠乳腺中MC的致癌性中并不重要。

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