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柯桠素对小鼠皮肤肿瘤的促癌机制

Mechanism of mouse skin tumor promotion by chrysarobin.

作者信息

DiGiovanni J, Decina P C, Prichett W P, Cantor J, Aalfs K K, Coombs M M

出版信息

Cancer Res. 1985 Jun;45(6):2584-9.

PMID:3986797
Abstract

The skin tumor-promoting ability of 1,8-dihydroxy-3-methyl-9-anthrone (chrysarobin) was compared with that of 12-O-tetradecanoylphorbol-13-acetate (TPA) and 1,8-dihydroxy-9-anthrone (anthralin) in SENCAR mice. Although dose-response comparisons indicated that chrysarobin was several orders of magnitude less potent than TPA for promoting papilloma formation, this anthrone was 1.5 to 2 times more potent than anthralin. Maximal papilloma responses were achieved by 15 weeks of promotion with TPA whereas at least 25 weeks of promotion were necessary to achieve maximal papilloma responses with chrysarobin or anthralin indicating marked differences in tumor latency between the two classes of compounds. Interestingly, at optimal promoting doses, chrysarobin gave a carcinoma response (22% with 0.3 carcinomas per mouse at 45 weeks) similar to that of TPA suggesting that this compound may be more efficient at promoting carcinomas than papillomas. In two-stage promotion experiments, chrysarobin was incapable of functioning independently as a Stage I or II promoter despite its complete promoting activity. Chrysarobin and TPA were compared at optimal promoting doses for their ability to induce: (a) skin edema, (b) epidermal hyperplasia, and (c) epidermal ornithine decarboxylase. In each case, distinct differences were noted between the two compounds. When taken together, the data support the hypothesis that anthracene-derived skin tumor promoters work at least in part by a mechanism different from the phorbol esters.

摘要

在SENCAR小鼠中,比较了1,8 - 二羟基 - 3 - 甲基 - 9 - 蒽酮(柯桠素)与12 - O - 十四烷酰佛波醇 - 13 - 乙酸酯(TPA)和1,8 - 二羟基 - 9 - 蒽酮(地蒽酚)的皮肤肿瘤促进能力。尽管剂量反应比较表明,柯桠素在促进乳头瘤形成方面的效力比TPA低几个数量级,但这种蒽酮的效力比地蒽酚高1.5至2倍。TPA促进15周可达到最大乳头瘤反应,而用柯桠素或地蒽酚则至少需要25周的促进才能达到最大乳头瘤反应,这表明两类化合物在肿瘤潜伏期上存在显著差异。有趣的是,在最佳促进剂量下,柯桠素产生的癌反应(45周时每只小鼠有0.3个癌,发生率为22%)与TPA相似,这表明该化合物在促进癌方面可能比促进乳头瘤更有效。在两阶段促进实验中,尽管柯桠素有完全的促进活性,但它不能独立作为I期或II期促进剂发挥作用。比较了柯桠素和TPA在最佳促进剂量下诱导以下情况的能力:(a)皮肤水肿,(b)表皮增生,以及(c)表皮鸟氨酸脱羧酶。在每种情况下,两种化合物之间都存在明显差异。综合来看,这些数据支持以下假设:蒽衍生的皮肤肿瘤促进剂至少部分通过一种不同于佛波酯的机制起作用。

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