Bioassay of diarylanilide yellow for possible carcinogenicity.

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Abstract

A bioassay of technical-grade diarylanilide yellow for possible carcinogenicity was conducted using Fischer 344 rats and B6C3F1 mice. Diarylanilide yellow was administered in the feed, at either of two concentrations, to groups of 50 male and 50 female animals of each species. The high and low dietary concentrations used in the chronic study for the male and female rats and mice were 5.0 and 2.5 percent, respectively, of the chemical in the feed. After a 78-week treatment period, observation of the rats continued for an additional 28 weeks and observation of the mice continued for an additional 19 weeks for high dose males and low and high dose females and 18 weeks for low dose males. For each species, 50 animals of each sex were placed on test as controls, and fed only the basal diet. The high concentration administered to both species in this study was the maximum recommended in the Guidelines for Carcinogen Bioassay in Small Rodents. These guidelines indicate that a chronic dietary level of 5 percent, or 50,000 ppm, should not be exceeded even when no signs of toxicity are observed during subchronic testing, except under special circumstances (e.g., when the compound is a major component of the human diet). No toxic effects were reported during subchronic testing and diarylanilide yellow did not qualify for exception; therefore, the highest permissible concentration (5 percent) was utilized in the chronic bioassay. The dietary concentrations of diarylanilide yellow administered during the chronic bioassay had no significant effect on survival or body weight gain in either species. Except for yellow staining and some isolated neoplasms, the only adverse clinical sign or pathologic lesion observed in treated rats or mice was basophilic cytoplasm changes in hepatocytes of treated rats. In both species the survival in all groups was adequate for statistical analysis of late-appearing tumors. No treatment-related increase in the incidence of neoplasms or nonneoplastic lesions was evident in treated rats or mice. A few unusual findings were observed in both species, including single cases of metastatic chordoma and osteogenic sarcoma in rats, and single cases of squamous-cell carcinoma of the ear, infiltrating duct carcinoma of the mammary gland, and subcutaneous mastocytoma in mice. The results of the study did not provide evidence for the carcinogenicity of diarylanilide yellow in Fischer 344 rats or B6C3F1 mice.

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二芳酰苯胺黄可能致癌性的生物测定。
采用Fischer 344大鼠和B6C3F1小鼠对技术级二芳酰苯胺黄进行了可能致癌性的生物测定。将二芳酰苯胺黄以两种浓度中的任意一种加入饲料中,每组50只雄性和50只雌性动物。在慢性研究中,雄性和雌性大鼠和小鼠的饮食中使用的高、低浓度分别是饲料中化学物质的5.0%和2.5%。78周的治疗期后,对大鼠的观察延长了28周,对高剂量雄性和低、高剂量雌性小鼠的观察延长了19周,对低剂量雄性小鼠的观察延长了18周。每个种属,雌雄各50只作为对照,只饲喂基础饲粮。本研究中对这两个物种施用的高浓度是《小型啮齿动物致癌物生物测定指南》中建议的最大浓度。这些指南表明,即使在亚慢性测试中没有观察到毒性迹象,也不应超过5%或50,000 ppm的慢性饮食水平,除非在特殊情况下(例如,当该化合物是人类饮食的主要成分时)。在亚慢性试验中未报告毒性作用,二芳酰苯胺黄不符合例外条件;因此,在慢性生物测定中使用最高允许浓度(5%)。在慢性生物测定期间,饮食中添加的二芳酰苯胺黄浓度对两种动物的生存或体重增加没有显著影响。除黄色染色和部分孤立肿瘤外,治疗大鼠或小鼠中观察到的不良临床体征或病理病变仅为治疗大鼠肝细胞嗜碱性细胞质改变。在这两个物种中,所有组的生存率都足以对晚期肿瘤进行统计分析。在接受治疗的大鼠或小鼠中,肿瘤或非肿瘤性病变的发生率没有明显的治疗相关增加。在这两个物种中都观察到一些不寻常的发现,包括大鼠的转移性脊索瘤和成骨性肉瘤的单个病例,以及小鼠的耳鳞状细胞癌、乳腺浸润导管癌和皮下肥大细胞瘤的单个病例。研究结果并未提供二芳酰苯胺黄对Fischer 344大鼠或B6C3F1小鼠致癌性的证据。
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