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柯桠素诱导SENCAR小鼠产生的乳头瘤的消退和进展特征

Regression and progression characteristics of papillomas induced by chrysarobin in SENCAR mice.

作者信息

Battalora M S, Conti C J, Aldaz C M, Slaga T J, Johnston D A, DiGiovanni J

机构信息

Department of Carcinogenesis, University of Texas, M.D. Anderson Cancer Center, Smithville 78957, USA.

出版信息

Carcinogenesis. 1996 May;17(5):955-60. doi: 10.1093/carcin/17.5.955.

Abstract

The present study was designed to test the effects of a free radical generating tumor promoter, chrysarobin (1,8-dihydroxy-3-methyl-9-anthrone), on the growth and progression of papillomas generated in the skin of SENCAR mice. In the first set of experiments, papillomas were generated by initiation with 6.4 microg of 7,12-dimethylbenz[a]anthracene (DMBA) followed by promotion with once-weekly applications of 52.8 microg chrysarobin for 10 weeks. The fate of individual papillomas was then monitored for a 20 week interval following cessation of promoter treatment. Five weeks after the cessation of chrysarobin treatment, the papilloma response reached a maximum of 13.2 papillomas/mouse. By the end of the 20 week interval 19% and 18% of the papillomas had regressed or coalesced respectively. A three-stage treatment protocol was also utilized to test the ability of chrysarobin to enhance the progression of pre-existing papillomas to squamous cell carcinomas (SCCs). In stage I, mice were initiated with 0.5 microg of DMBA. In stage II, mice were promoted with twice-weekly applications of 1 or 2 microg of 12-0-tetradecanoylphorbol-13-acetate (TPA) for 15 weeks. Then, in stage III, mice were treated with acetone, TPA (1 or 2 microg), chrysarobin (52.8 microg) or benzoyl peroxide (BzPo; 20 mg) for the next 45 weeks. The mean number of papillomas per mouse at plateau was very similar for all groups. The carcinoma incidence was also similar for all groups regardless of the treatment protocol used, as was the mean number of carcinomas per mouse. The ratio of papillomas that converted to SCCs in mice treated with chrysarobin during stage III was not significantly different from the acetone controls or any of the other treatment groups (P > 0.05, Kruskal-Wallis analysis). In addition, BzPo did not enhance the progression of papillomas to SCCs under the current experimental conditions. Collectively, the results indicate that papillomas promoted by chrysarobin have growth properties similar to those promoted by TPA under similar experimental conditions. Furthermore, despite its ability to generate free radical intermediates, chrysarobin does not enhance the malignant progression of pre-existing papillomas induced by TPA treatment.

摘要

本研究旨在测试一种自由基生成性肿瘤促进剂柯桠素(1,8 - 二羟基 - 3 - 甲基 - 9 - 蒽酮)对SENCAR小鼠皮肤乳头状瘤生长和进展的影响。在第一组实验中,通过用6.4微克的7,12 - 二甲基苯并[a]蒽(DMBA)启动,随后每周一次应用52.8微克柯桠素进行10周的促进,来生成乳头状瘤。然后在停止促进剂处理后的20周间隔内监测各个乳头状瘤的转归。在停止柯桠素处理5周后,乳头状瘤反应达到最大值,即每只小鼠有13.2个乳头状瘤。到20周间隔结束时,分别有19%和18%的乳头状瘤消退或融合。还采用了三阶段治疗方案来测试柯桠素促进已存在的乳头状瘤发展为鳞状细胞癌(SCC)的能力。在第一阶段,用0.5微克的DMBA启动小鼠。在第二阶段,每周两次应用1或2微克的12 - O - 十四烷酰佛波醇 - 13 - 乙酸酯(TPA)对小鼠进行促进,持续15周。然后,在第三阶段,在接下来的45周内,用丙酮、TPA(1或2微克)、柯桠素(52.8微克)或过氧化苯甲酰(BzPo;20毫克)对小鼠进行处理。所有组在平台期每只小鼠的乳头状瘤平均数量非常相似。无论使用何种治疗方案,所有组的癌发生率以及每只小鼠的癌平均数量也相似。在第三阶段用柯桠素处理的小鼠中,转化为SCC的乳头状瘤比例与丙酮对照组或任何其他治疗组相比无显著差异(P>0.05,Kruskal - Wallis分析)。此外,在当前实验条件下,BzPo并未促进乳头状瘤发展为SCC。总体而言,结果表明在相似实验条件下,由柯桠素促进的乳头状瘤具有与由TPA促进的乳头状瘤相似的生长特性。此外,尽管柯桠素有能力生成自由基中间体,但它并不会促进由TPA处理诱导的已存在乳头状瘤的恶性进展。

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