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大鼠前列腺及其他靶器官中肿瘤发生率随3,2'-二甲基-4-氨基联苯给药剂量和给药持续时间的变化而变化。

Variation in tumor yield in the prostate and other target organs of the rat in response to varied dosage and duration of administration of 3,2'-dimethyl-4-aminobiphenyl.

作者信息

Ito N, Shirai T, Tagawa Y, Nakamura A, Fukushima S

机构信息

First Department of Pathology, Nagoya City University Medical School, Japan.

出版信息

Cancer Res. 1988 Aug 15;48(16):4629-32.

PMID:3396013
Abstract

The effects of varying dosages of 3,2'-dimethyl-4-aminobiphenyl (DMAB) in combination with cyclic dietary administration of ethinyl estradiol (EE) on induction of prostate carcinoma were investigated in male F344 rats. Animals received repeated treatment with 0.75 ppm of EE for 3 wk with intervals of 2 wk on basal diet. The cycle was repeated 10, 5, and 3 times in Groups 1, 2, and 3, respectively, a single s.c. injection of DMAB being given 2 days after each change to basal diet at a dose of 50 mg/kg of body weight in Group 1, 100 mg/kg of body weight in Group 2, and 167 mg/kg of body weight in Group 3. With this dosing schedule, the total dose of DMAB (500 mg/kg of body weight) per rat was the same in each group. Subsequent to the last treatment with EE, all rats were given basal diet until the end of the experiment (Wk 60) when all surviving animals were sacrificed for histological examination. Carcinoma of the prostate was found in 58.6, 45.0, and 25.9% of rats surviving for 60 wk in Groups 1 to 3, respectively, the incidences of atypical hyperplasia being 86.2, 85.0, and 74.1%. However, tumors of the small and large intestines, preputial gland, and pancreas developed in a dosage-dependent manner, the largest incidences being found in the group given 167 mg of carcinogen 3 times. Thus the present experiment confirmed that administration of DMAB combined with cyclic treatment with EE induces a high incidence of prostate carcinoma in rats and demonstrated that a low dosage of DMAB given over a long period is superior to a high dosage over a short period for specific induction of prostate lesions.

摘要

研究了不同剂量的3,2'-二甲基-4-氨基联苯(DMAB)与炔雌醇(EE)周期性饮食给药联合使用对雄性F344大鼠前列腺癌诱导的影响。动物在基础饮食上,每隔2周接受一次0.75 ppm EE的重复治疗,持续3周。第1、2和3组分别重复该周期10次、5次和3次,每次改为基础饮食2天后,第1组皮下注射一次剂量为50 mg/kg体重的DMAB,第2组为100 mg/kg体重,第3组为167 mg/kg体重。按照这种给药方案,每组每只大鼠的DMAB总剂量(500 mg/kg体重)相同。在用EE进行最后一次治疗后,所有大鼠均给予基础饮食直至实验结束(第60周),此时所有存活动物均被处死进行组织学检查。在第1至3组存活60周的大鼠中,分别有58.6%、45.0%和25.9%发生了前列腺癌,非典型增生的发生率分别为86.2%、85.0%和74.1%。然而,小肠和大肠、包皮腺和胰腺的肿瘤呈剂量依赖性发展,在接受3次167 mg致癌物的组中发生率最高。因此,本实验证实DMAB与EE周期性治疗联合给药可诱导大鼠前列腺癌的高发生率,并表明长期给予低剂量的DMAB在特异性诱导前列腺病变方面优于短期给予高剂量的DMAB。

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