可能致癌性的磷胺生物测定。

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引用次数: 0

摘要

用奥斯本-孟德尔大鼠和B6C3F1小鼠进行了技术级磷酰胺可能致癌性的生物测定。试验材料以两种剂量(80或160 ppm)中的一种加入饲料,分别喂给50只大鼠和50只雌雄小鼠。给药80周,不给药30周、31周;低剂量雄性小鼠先喂养71周,再观察19周;高剂量雄性小鼠先喂养62周,再观察28周;低剂量和高剂量雌性小鼠分别饲喂80周,观察10周和11周。配对的对照组由每性别10只未治疗的大鼠或10只未治疗的小鼠组成;混合对照组由匹配的对照组和85只雄性和85只雌性未经处理的大鼠或80只雄性和80只雌性未经处理的小鼠组成,这些小鼠来自其他8种测试化学物质的类似生物测定。所有存活的大鼠在110周或111周时处死;所有存活的小鼠在90周或91周时被杀死。在给药的大鼠和小鼠中观察到高兴奋性和震颤,这是磷酰胺毒性的两种适应症。然而,两种物种的所有组中有足够数量的人有发展为晚期肿瘤的风险。在雄性大鼠中,脾脏血管瘤和血管肉瘤的合并发病率呈剂量相关趋势,具有统计学意义(P=0.012)。然而,与匹配对照组的比较不显著,本实验室对该菌株未经治疗的雄性的历史记录显示肿瘤发病率为6/240(3%),个别对照组的发病率高达3/9(33%)和2/9(22%),而本研究中高剂量组的发病率为5/49(10%)。女性未见血管瘤或血管性肉瘤。在雌性大鼠中,当合并对照组与给药组比较时,c细胞腺瘤和甲状腺癌的科克伦-阿米蒂奇检验的剂量相关趋势显著(P=0.003)。当低剂量女性(P=0.003)和高剂量女性(P=0.004)与合并对照直接比较时,这些肿瘤的发生率也很显著。然而,本实验室的历史记录显示,该品系雌性大鼠未经治疗的雌性大鼠肿瘤发生率为16/235(7%),个别对照组的发病率高达3/9(33%)和3/10 (30%);因此,这些数据被认为是边缘的,不足以建立肿瘤与化学物质施用之间的联系。在男性中,这些肿瘤的发病率没有统计学意义。在小鼠实验中,给药动物的肿瘤发生率没有高于对照组。在本实验条件下,技术级磷酰胺对B6C3F1小鼠无致癌性。在奥斯本-孟德尔大鼠的生物测定中获得的数据不足以解释技术级磷在该物种中具有致癌性。
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Bioassay of phosphamidon for possible carcinogenicity.

A bioassay of technical-grade phosphamidon for possible carcinogenicity was conducted using Osborne-Mendel rats and B6C3F1 mice. The test material was administered in feed to 50 rats and 50 mice of each sex at one of two doses, either 80 or 160 ppm. The rats were fed the test chemical for 80 weeks, then observed without compound administration for 30 or 31 weeks; the low-dose male mice were fed for 71 weeks, then observed for 19 weeks; the high-dose male mice were fed for 62 weeks, then observed for 28 weeks; and the low- and high-dose female mice were fed for 80 weeks, then observed for 10 or 11 weeks. Matched controls consisted of groups of 10 untreated rats or 10 untreated mice of each sex; pooled controls consisted of the matched controls combined with 85 male and 85 female untreated rats or 80 male and 80 female untreated mice from similar bioassays of eight other test chemicals. All surviving rats were killed at 110 or 111 weeks; all surviving mice were killed at 90 or 91 weeks. Hyperexcitability and tremors, both indications of phosphamidon toxicity, were observed in dosed rats and mice. However, sufficient numbers of all groups of both species were at risk for the development of late-appearing tumors. In male rats, the combined incidence of hemangiomas and hemangiosarcomas in the spleen showed a statistically significant (P=0.012) dose-related trend. However, the comparison with matched controls was not significant, and the historical records of this laboratory on untreated males of this strain show a tumor incidence of 6/240 (3%) with incidences in individual control groups as high as 3/9 (33%)and 2/9 (22%), compared with 5/49 (10%) seen in the high-dose group in this study. No hemangiomas or hemangiosarcomas were found in the females. In female rats, the Cochran-Armitage test for dose-related trend was significant (P=0.003) for C-cell adenomas and carcinomas of the thyroid when pooled controls were compared with the dosed groups. The incidences of these tumors were also significant when low-dose females (P=0.003) and high-dose females (P=0.004) were compared directly with pooled controls. However, the historical records of this laboratory show a tumor incidence of 16/235 (7%) in untreated female rats of this strain of female rats, with incidences in individual control groups as high as 3/9 (33%) and 3/10 (30%); these data are therefore considered marginal and insufficient to establish an association between the tumors and administration of the chemical. In males, the incidence of these tumors was not statistically significant. In mice, no tumor occurred at a higher incidence in dosed animals than in controls. It is concluded that under the conditions of this bioassay, technical-grade phosphamidon was not carcinogenic for B6C3F1 mice. The data obtained in this bioassay with Osborne-Mendel rats are insufficient to allow the interpretation that technical-grade phosphamidon is carcinogenic in this species.

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