Bioassay of nithiazide for possible carcinogenicity.

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Abstract

The bioassay of nithiazide for possible carcinogenicity was conducted using Fischer 344 rats and B6C3F1 mice. Nithiazide was administered in the diet, at either of two concentrations, to groups of 50 male and 50 female animals of each species. The high and low concentrations of nithiazide utilized were, respectively, 1,250 and 625 ppm for rats and 5,000 and 2,500 ppm for mice. Dosed rats received feed containing nithiazide for 38 weeks, and as a result of a shortage of nithiazide, the animals were not fed the dosed feed for the next 9 weeks. The dosed feed diet was then resumed and continued for 56 weeks, after which time a 1-week observation period followed. Dosed mice received feed containing nithiazide for 61 weeks and, due to a shortage of nithiazide, the animals were not fed dosed feed for the next 9 weeks. The dosed feed diet was then resumed and continued for 33 weeks, followed by a 1-week observation period. Twenty animals of each sex and species were placed on test as controls. In both species, adequate numbers of animals survived sufficiently long to be at risk from late-developing tumors. There was no significant positive association between dosage and mortality for either rats or mice. Compound-related mean body weight depression occurred in both sexes of each species. Statistically significant incidences of hepatocellular adenomas and carcinomas were found in high dose male mice but not in female mice. Although the increased incidences of these tumors in dosed female mice were not statistically significant, the evidence presented was strongly suggestive of carcinogenicity to the liver in female B6C3F1 mice. Statistically significant increased incidences of a combination of mammary and skin fibroadenomas and cystadenomas NOS were found in the high dose female rats. No unusual tumors were observed in either species. Under the conditions of this bioassay, nithiazide was carcinogenic in male and probably female B6C3F1 mice, causing a combination of hepatocellular carcinomas and hepatocellular adenomas. Nithiazide was also carcinogenic in female Fischer 344 rats, causing an increase in the incidence of mammary neoplasms. The compound was not carcinogenic in male Fischer 344 rats.

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氮噻嗪可能致癌性的生物测定。
采用Fischer 344大鼠和B6C3F1小鼠进行了硝噻嗪可能致癌性的生物测定。每组50只雄性和50只雌性动物在饮食中以两种浓度中的任意一种给予噻嗪。大鼠使用的高、低浓度硝噻嗪分别为1250和625 ppm,小鼠使用的高、低浓度硝噻嗪分别为5000和2500 ppm。给药大鼠喂食含有氮噻嗪的饲料38周,由于氮噻嗪缺乏,动物在接下来的9周内没有喂食给药饲料。恢复加药饲粮,连续饲喂56周,然后进行1周的观察期。给药小鼠喂食含有噻嗪的饲料61周,由于缺乏噻嗪,动物在接下来的9周内没有喂食。恢复加药饲粮,持续饲喂33周,然后进行1周的观察期。各性别、各物种各20只作为对照进行试验。在这两个物种中,足够数量的动物存活了足够长的时间,从而有可能患上晚期肿瘤。大鼠和小鼠的剂量和死亡率之间没有显著的正相关。化合物相关的平均体重下降发生在每个物种的两性中。在高剂量雄性小鼠中发现肝细胞腺瘤和癌的发生率有统计学意义,而在雌性小鼠中没有。虽然这些肿瘤在给药雌性小鼠中的发病率增加没有统计学意义,但所提供的证据强烈提示雌性B6C3F1小鼠的肝脏具有致癌性。在高剂量雌性大鼠中,乳腺和皮肤纤维腺瘤及囊腺瘤NOS的发生率显著增加。两种动物均未见异常肿瘤。在本生物试验条件下,硝噻嗪对雄性,也可能是雌性B6C3F1小鼠具有致癌性,引起肝细胞癌和肝细胞腺瘤的结合。ni噻嗪在雌性Fischer 344大鼠中也具有致癌性,导致乳腺肿瘤的发生率增加。该化合物对雄性Fischer 344大鼠无致癌性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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