胡椒酰丁醇可能致癌性的生物测定(CAS No. 51-03-6)。

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引用次数: 0

摘要

通过给Fischer 344大鼠和B6C3F1小鼠喂食饲料中的试验化学品,对技术级胡椒酰丁醇进行了可能致癌性的生物测定。每组50只雌雄老鼠,以两种剂量(5000 ppm或10000 ppm)中的一种给药,持续107周。配对的对照组包括20只未治疗的大鼠,雌雄各一只。所有存活的老鼠在给药结束时被杀死。每组50只雌雄老鼠最初被注射胡椒酰丁醇,剂量为2500或5000 ppm。第30周后,小鼠的剂量分别减少到500ppm和2000ppm,并以降低的剂量持续给药82周。小鼠的时间加权平均剂量为1,036或2,804 ppm。配对的对照组由雌雄各20只未经治疗的老鼠组成。所有存活的老鼠在给药期结束时被杀死。各给药组大鼠和小鼠的平均体重均低于相应的对照组,体重的下降与剂量有关。大鼠和小鼠的存活率不受丁二醇胡椒酯的影响,在生物测定的第90周,所有组的存活率都在80%或更高;因此,足够数量的剂量大鼠和对照大鼠以及雌雄小鼠都有发生晚期肿瘤的风险。雌性大鼠淋巴瘤发生率与剂量相关(P=0.007);直接比较,高剂量组肿瘤发生率高于对照组(对照组1/20,低剂量组7/50,高剂量组15/50)(P=0.020)。然而,在同一实验室的历史对照雌性Fischer 344大鼠中,淋巴瘤、白血病和网状蛋白的发病率为19/191(10%)。这些历史对照组包括淋巴瘤或白血病发生率为7/20(35%)和6/20(30%)的动物。因此,在本生物测定的对照雌性大鼠中,淋巴瘤的发病率可能异常低,而在给药组中较高发病率的发生不能与给药胡椒酰丁醇明确相关。在雄性小鼠中,泪腺腺瘤的发生率与剂量相关(P=0.023),但在直接比较中,各剂量组的发生率均不显著高于对照组(对照组0/20,低剂量0/49,高剂量4/50);因此,这种肿瘤在雄性小鼠中的发生与试验化学物质的施用没有明确的关系。结论:在本实验条件下,胡椒酰丁醇对Fischer 344大鼠和B6C3F1小鼠均无致癌性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Bioassay of piperonyl butoxide for possible carcinogenicity (CAS No. 51-03-6).

A bioassay of technical-grade piperonyl butoxide for possible carcinogenicity was conducted by administering the test chemical in feed to Fischer 344 rats and B6C3F1 mice. Groups of 50 rats of each sex were administered piperonyl butoxide in the diet at one of two doses, either 5,000 or 10,000 ppm, for 107 weeks. Matched controls consisted of 20 untreated rats of each sex. All surviving rats were killed at the end of the period of administration of the test chemical. Groups of 50 mice of each sex were initially administered piperonyl butoxide at one of two doses, either 2,500 or 5,000 ppm. After week 30, the doses for the mice were reduced to 500 and 2,000 ppm, respectively, and administration of the test chemical at the lowered doses was continued for 82 weeks. The time-weighted average doses for the mice were either 1,036 or 2,804 ppm. Matched controls consisted of 20 untreated mice of each sex. All surviving mice were killed at the end of the period of administration of the test chemical. Mean body weights of dosed groups of rats and mice of each sex were lower than those of corresponding control groups, and the depressions in body weights were dose related. Survival of the rats and mice was unaffected by the piperonyl butoxide and was 80% or greater in all groups at week 90 of the bioassay; thus, sufficient numbers of dosed and control rats and mice of each sex were at risk for the development of late-appearing tumors. In female rats, lymphomas occurred at incidences that were dose related (P=0.007); in a direct comparison, the incidence of the tumor in the high-dose group was higher (P=0.020) than that in the control group (controls 1/20, low-dose 7/50, high-dose 15/50). However, the incidence of lymphomas, leukemias, and reticuloses in historical-control female Fischer 344 rats at the same laboratory was 19/191 (10%). These historical-control groups include one with an incidence of animals with lymphoma or leukemia of 7/20 (35%) and another with an incidence of 6/20 (30%). Thus, the incidence of lymphomas in the control female rats of the present bioassay may have been abnormally low, and the occurrence of the higher incidence in the dosed groups cannot be clearly related to administration of piperonyl butoxide. In the male mice, adenomas of the lacrimal gland occurred at incidences that were dose related (P=0.023), but in direct comparisons the incidences in the individual dosed groups were not significantly higher than that in the control group (controls 0/20, low-dose 0/49, high-dose 4/50); thus, the occurrence of this tumor in the male mice was not clearly related to administration of the test chemical. It is concluded that under the conditions of this bioassay, piperonyl butoxide was not carcinogenic for Fischer 344 rats or B6C3F1 mice.

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