Bioassay of hydrazobenzene for possible carcinogenicity.

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Abstract

A bioassay of technical-grade hydrazobenzene for possible carcinogenicity was conducted using Fischer 344 rats and B6C3F1 mice. Hydrazobenzene was administered in the feed, at either of two concentrations, to groups of 50 male and 47 to 50 females animals of each species. The time-weighted average dietary concentrations used in the rat bioassay were 0.008, 0.03, 0.004, and 0.01 percent for low dose males, high dose males, low dose females, and high dose females, respectively. The time-weighted average dietary concentrations used in the mouse bioassay were 0.008, 0.04, 0.004, and 0.04 percent for low dose males, high dose males, low dose females, and high dose females, respectively. After a 78-week period of compound administration, observation of the rats continued for an additional 28 to 30 weeks and observation of the mice continued for an additional 17 or 18 weeks. For each species, 47 to 50 animals of each sex were placed on test as controls. In both, species, adequate numbers of animals in all groups survived sufficiently long to be at risk from late-appearing tumors. The incidence of hepatocellular carcinomas was significantly increased in dosed male rats and the incidence of neoplastic nodules of the liver was significantly increased in dosed female rats. A significant increase in the combined incidence of squamous-cell carcinomas or squamous-cell papillomas of the Zymbal's gland, the ear canal, or the skin of the ear was observed among high dose male rats. A significant increase in mammary adenocarcinomas was observed among dosed female rats. The incidence of hepatocellular carcinomas was significantly increased among female mice, but no significant increase in liver tumors was observed among male mice. Under the conditions of this bioassay, hydrazobenzene was carcinogenic to Fischer 344 rats of both sexes, causing increased incidences of hepatocellular carcinoma and Zymbal's gland squamous-cell neoplasms in male rats, neoplastic nodules of the liver in female rats, and mammary adenocarcinomas in female rats. Hydrazobenzene was also carcinogenic to female B6C3F1 mice, causing an increased incidence of hepatocellular carcinomas. The compound was not carcinogenic to male B6C3F1 mice.

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对苯苯可能致癌性的生物测定。
采用Fischer 344大鼠和B6C3F1小鼠进行了技术级苯的致癌性生物测定。在饲料中以两种浓度中的任何一种给药,每组50只雄性动物和47至50只雌性动物。低剂量雄鼠、高剂量雄鼠、低剂量雌鼠和高剂量雌鼠的时间加权平均饮食浓度分别为0.008%、0.03%、0.004%和0.01%。在小鼠生物测定中,低剂量雄性、高剂量雄性、低剂量雌性和高剂量雌性的时间加权平均饮食浓度分别为0.008%、0.04%、0.004%和0.04%。在78周的复合给药期后,对大鼠的观察再持续28至30周,对小鼠的观察再持续17或18周。对每个物种,每个性别的47 - 50只动物作为对照进行试验。在这两个物种中,所有群体中都有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。给药雄性大鼠肝细胞癌的发生率显著增加,给药雌性大鼠肝脏肿瘤结节的发生率显著增加。在高剂量雄性大鼠中,观察到舌腺、耳道或耳皮肤的鳞状细胞癌或鳞状细胞乳头状瘤的合并发病率显著增加。在给药的雌性大鼠中观察到乳腺腺癌的显著增加。雌性小鼠的肝细胞癌发生率显著增加,而雄性小鼠的肝脏肿瘤发生率无显著增加。在本实验条件下,肼苯对雌雄Fischer 344大鼠均具有致癌性,雄性大鼠肝细胞癌、淋巴腺鳞状细胞瘤、雌性大鼠肝脏肿瘤结节、雌性大鼠乳腺腺癌的发生率均增加。对雌性B6C3F1小鼠也有致癌作用,导致肝细胞癌的发病率增加。该化合物对雄性B6C3F1小鼠无致癌性。
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