盐酸非那吡啶可能致癌性的生物测定。

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Mean body weights of the dosed rats and mice of each sex were consistently lower than those of corresponding control animals, and the depressions in mean body weight were dose related. Mortality in the groups of rats and mice did not, however, show dose-related trends, and sufficient numbers of animals of both dosed and control groups were at risk for the development of late-appearing tumors. In male rats, adenomas or adenocarcinomas of the large intestine (colon or rectum) occurred at incidences having a significant dose-related trend (P=0.015). The direct comparison of the incidences in each of the dosed groups with that in the control group was not significant (controls 0/14, low-dose 4/34, high-dose 8/35). In the females, 3/33 low-dose and 5/32 high-dose animals, but no control animals, had this tumor. In addition, sarcomas were observed in the colon of one low-dose male and one high-dose female. 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引用次数: 0

摘要

通过给Fischer 344大鼠和B6C3F1小鼠喂食饲料,对盐酸非那唑吡啶可能的致癌性进行了生物测定。每组35只大鼠和35只小鼠按下列剂量之一服用盐酸苯那吡啶,大鼠服用剂量为3700或7500 ppm,小鼠服用剂量为600或1200 ppm。给大鼠服用78周,然后再观察26或27周;小鼠服用该化学物质80周,然后再观察25-27周。配对的对照组包括15只未治疗的大鼠和15只未治疗的小鼠。所有存活的大鼠在104或105周时被杀死,所有存活的小鼠在105-107周时被杀死。各性别大鼠和小鼠的平均体重均低于相应的对照动物,平均体重的下降与剂量有关。然而,大鼠和小鼠组的死亡率没有显示出剂量相关的趋势,并且剂量组和对照组的足够数量的动物都有发生晚期肿瘤的风险。在雄性大鼠中,腺瘤或大肠(结肠或直肠)腺癌的发生率呈显著的剂量相关趋势(P=0.015)。各给药组与对照组发病率直接比较无统计学意义(对照组0/14,低剂量4/34,高剂量8/35)。在雌性动物中,3/33的低剂量和5/32的高剂量动物有这种肿瘤,但没有对照动物。此外,在一名低剂量男性和一名高剂量女性的结肠中观察到肉瘤。实验室历史记录显示260例女性未发生大肠腺瘤或腺癌,260例男性仅发生1例腺瘤性息肉。假设自发发生率为1/261(0.038%),且肿瘤呈二项分布,则高剂量组男性和女性的发生率均显著(P
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Bioassay of phenazopyridine hydrochloride for possible carcinogenicity.

A bioassay of phenazopyridine hydrochloride for possible carcinogenicity was conducted by administering the test chemical in feed to Fischer 344 rats and B6C3F1 mice. Groups of 35 rats and 35 mice of each sex were administered phenazopyridine hydrochloride at one of the following doses, either 3,700 or 7,500 ppm for rats and either 600 or 1,200 ppm for mice. The rats were administered the chemical for 78 weeks, then observed for 26 or 27 additional weeks; the mice were administered the chemical for 80 weeks, then observed for 25-27 additional weeks. Matched controls consisted of 15 untreated rats and 15 untreated mice of each sex. All surviving rats were killed at 104 or 105 weeks, all surviving mice at 105-107 weeks. Mean body weights of the dosed rats and mice of each sex were consistently lower than those of corresponding control animals, and the depressions in mean body weight were dose related. Mortality in the groups of rats and mice did not, however, show dose-related trends, and sufficient numbers of animals of both dosed and control groups were at risk for the development of late-appearing tumors. In male rats, adenomas or adenocarcinomas of the large intestine (colon or rectum) occurred at incidences having a significant dose-related trend (P=0.015). The direct comparison of the incidences in each of the dosed groups with that in the control group was not significant (controls 0/14, low-dose 4/34, high-dose 8/35). In the females, 3/33 low-dose and 5/32 high-dose animals, but no control animals, had this tumor. In addition, sarcomas were observed in the colon of one low-dose male and one high-dose female. The laboratory historical records showed no incidence of adenomas or adenocarcinomas of the large intestine in 260 females and only one adenomatous polyp in 260 males. Assuming a spontaneous incidence of 1/261 (0.038%) and a binomial distribution of such tumors, the occurrence seen in the male and female high-dose groups are both significantly (P<0.001) different from the expected value. Thus, these tumors are considered to be related to administration of the test chemical. In female mice, the combined incidence of hepatocellular adenomas and carcinomas showed a significant dose-related trend (P=0.002), and the incidence in the high-dose group was significant (P=0.003) when compared with that in the control group (controls 2/15, low-dose 11/34, high-dose 19/32). The incidence of hepatocellular carcinomas, considered alone, also was significant in female mice, showing a dose-related trend (P=0.010) and a P value of 0.039 for the comparison of the high-dose group with the control group. In the males, the combined incidence of hepatocellular adenomas and carcinomas was not significant. It is concluded that under the conditions of this bioassay, phenazopyridine hydrochloride was carcinogenic in Fischer 344 rats, inducing adenocarcinomas of the colon in both males and females. Although phenazopyridine hydrochloride was not carcinogenic in male B6C3F1 mice, the chemical was carcinogenic in females, inducing hepatocellular adenomas and carcinomas.

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