S Mitsunaga, M Clapper, S Litwin, P Watts, B Bauer, A J Klein-Szanto
{"title":"二氟甲基鸟氨酸(DFMO)对苯并(a)芘诱发小鼠皮肤鳞状细胞癌的化学预防作用。","authors":"S Mitsunaga, M Clapper, S Litwin, P Watts, B Bauer, A J Klein-Szanto","doi":"","DOIUrl":null,"url":null,"abstract":"<p><p>The effect of the chemopreventive agent D,L-alpha-difluoromethylornithine (DFMO) on the incidence of skin squamous cell carcinoma was studied in SENCAR mice treated weekly with topical applications of benzo(a)pyrene (B(a)P) (0.15 mmol, 2 x /week) on the dorsal skin. Animals were randomized to receive either chow or chow supplemented with DFMO (1 g/1 kg) and studied at 10, 15, 20, 25, and 30 weeks of B(a)P treatment. Morphometric analyses at each timepoint evaluated the epidermal thickness (ET) and the number of epidermal nucleated layers (NL). The ET increased from 12-17 microns as early as 10 weeks after B(a)P treatment, reaching 22 microns at 20 weeks, and 27 microns at 25 weeks (130% increase). The NL also increased markedly. A relatively modest increase in ET was observed in animals treated with B(a)P and DFMO (16% at 15 weeks, 53% at 20 weeks, and 85% at 25 weeks) as compared to controls. The relative increase in NL showed a similar pattern. Although extensive epidermal hyperplasia was seen early, clear-cut focal premalignant lesions were not identifiable before week 20 of B(a)P treatment. At 20 weeks, the most frequently noted focal premalignant lesions in carcinogen-treated animals (without DFMO) were moderate dysplasias. At 25 and 30 weeks, a large increase was seen in the incidence of more advanced dysplastic lesions and invasive carcinomas. In the group treated with B(a)P and DFMO, a marked reduction in the number of carcinomas was observed at 25 and 30 weeks. At 25 weeks, DFMO reduced tumor yield from 5.8 to 3.2 carcinomas per mouse. At 30 weeks, the reduction was from 13.1 to 5.7 carcinomas per mouse (57% reduction). Collectively, these data emphasize the strong chemopreventive effect of DFMO against tumors in the mouse skin complete carcinogenesis model, as indicated by the reduction of overall skin tumor incidence and the decreased epidermal hyperplasia in DFMO-treated animals. Morphometrically defined increases in ET and NL can be used as early biomarkers of DFMO chemoprevention in mouse skin tumorigenesis.</p>","PeriodicalId":77196,"journal":{"name":"Journal of cellular biochemistry. 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Morphometric analyses at each timepoint evaluated the epidermal thickness (ET) and the number of epidermal nucleated layers (NL). The ET increased from 12-17 microns as early as 10 weeks after B(a)P treatment, reaching 22 microns at 20 weeks, and 27 microns at 25 weeks (130% increase). The NL also increased markedly. A relatively modest increase in ET was observed in animals treated with B(a)P and DFMO (16% at 15 weeks, 53% at 20 weeks, and 85% at 25 weeks) as compared to controls. The relative increase in NL showed a similar pattern. Although extensive epidermal hyperplasia was seen early, clear-cut focal premalignant lesions were not identifiable before week 20 of B(a)P treatment. At 20 weeks, the most frequently noted focal premalignant lesions in carcinogen-treated animals (without DFMO) were moderate dysplasias. At 25 and 30 weeks, a large increase was seen in the incidence of more advanced dysplastic lesions and invasive carcinomas. In the group treated with B(a)P and DFMO, a marked reduction in the number of carcinomas was observed at 25 and 30 weeks. At 25 weeks, DFMO reduced tumor yield from 5.8 to 3.2 carcinomas per mouse. At 30 weeks, the reduction was from 13.1 to 5.7 carcinomas per mouse (57% reduction). Collectively, these data emphasize the strong chemopreventive effect of DFMO against tumors in the mouse skin complete carcinogenesis model, as indicated by the reduction of overall skin tumor incidence and the decreased epidermal hyperplasia in DFMO-treated animals. Morphometrically defined increases in ET and NL can be used as early biomarkers of DFMO chemoprevention in mouse skin tumorigenesis.</p>\",\"PeriodicalId\":77196,\"journal\":{\"name\":\"Journal of cellular biochemistry. 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引用次数: 0
摘要
研究了化学预防剂D, l - α -二氟甲基鸟氨酸(DFMO)对SENCAR小鼠皮肤鳞状细胞癌发生率的影响,每周局部应用苯并(a)芘(B(a)P) (0.15 mmol, 2 x /周)于背部皮肤。实验动物随机分为两组,一组饲喂饲料,另一组饲喂添加DFMO (1 g/1 kg)的饲料,分别于B(a)P处理10、15、20、25和30周进行研究。每个时间点的形态计量学分析评估了表皮厚度(ET)和表皮有核层(NL)的数量。早在B(a)P处理10周后,ET就从12-17微米增加,20周时达到22微米,25周时达到27微米(增加130%)。NL也显著增加。与对照组相比,经B(A)P和DFMO处理的动物ET有相对适度的增加(15周时16%,20周时53%,25周时85%)。NL的相对增加也表现出类似的模式。虽然早期可见广泛的表皮增生,但在B(a)P治疗的第20周之前,未发现明确的局灶性癌前病变。在20周时,经致癌物处理的动物(无DFMO)最常见的局灶性癌前病变是中度发育不良。在25周和30周时,晚期发育不良病变和浸润性癌的发生率显著增加。在接受B(a)P和DFMO治疗的组中,在25周和30周观察到肿瘤数量明显减少。在25周时,DFMO将每只小鼠的肿瘤产量从5.8个减少到3.2个。在30周时,每只小鼠从13.1个癌减少到5.7个癌(减少57%)。综上所述,这些数据强调了DFMO对小鼠皮肤完全癌变模型中肿瘤的强大化学预防作用,正如DFMO处理的动物皮肤肿瘤总体发病率降低和表皮增生减少所表明的那样。形态计量学定义的ET和NL的增加可以作为DFMO化学预防小鼠皮肤肿瘤发生的早期生物标志物。
Chemopreventive effect of difluoromethylornithine (DFMO) on mouse skin squamous cell carcinomas induced by benzo(a)pyrene.
The effect of the chemopreventive agent D,L-alpha-difluoromethylornithine (DFMO) on the incidence of skin squamous cell carcinoma was studied in SENCAR mice treated weekly with topical applications of benzo(a)pyrene (B(a)P) (0.15 mmol, 2 x /week) on the dorsal skin. Animals were randomized to receive either chow or chow supplemented with DFMO (1 g/1 kg) and studied at 10, 15, 20, 25, and 30 weeks of B(a)P treatment. Morphometric analyses at each timepoint evaluated the epidermal thickness (ET) and the number of epidermal nucleated layers (NL). The ET increased from 12-17 microns as early as 10 weeks after B(a)P treatment, reaching 22 microns at 20 weeks, and 27 microns at 25 weeks (130% increase). The NL also increased markedly. A relatively modest increase in ET was observed in animals treated with B(a)P and DFMO (16% at 15 weeks, 53% at 20 weeks, and 85% at 25 weeks) as compared to controls. The relative increase in NL showed a similar pattern. Although extensive epidermal hyperplasia was seen early, clear-cut focal premalignant lesions were not identifiable before week 20 of B(a)P treatment. At 20 weeks, the most frequently noted focal premalignant lesions in carcinogen-treated animals (without DFMO) were moderate dysplasias. At 25 and 30 weeks, a large increase was seen in the incidence of more advanced dysplastic lesions and invasive carcinomas. In the group treated with B(a)P and DFMO, a marked reduction in the number of carcinomas was observed at 25 and 30 weeks. At 25 weeks, DFMO reduced tumor yield from 5.8 to 3.2 carcinomas per mouse. At 30 weeks, the reduction was from 13.1 to 5.7 carcinomas per mouse (57% reduction). Collectively, these data emphasize the strong chemopreventive effect of DFMO against tumors in the mouse skin complete carcinogenesis model, as indicated by the reduction of overall skin tumor incidence and the decreased epidermal hyperplasia in DFMO-treated animals. Morphometrically defined increases in ET and NL can be used as early biomarkers of DFMO chemoprevention in mouse skin tumorigenesis.
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