2,4,6-三氯苯酚可能致癌性的生物测定。

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引用次数: 0

摘要

通过给F344大鼠和B6C3F1小鼠喂食饲料,对2,4,6-三氯酚进行了可能致癌性的生物测定。每组各50只雌雄老鼠,以两种剂量(5000或10000 ppm)中的一种注射2,4,6-三氯苯酚,持续106或107周。配对的对照组包括20只未治疗的大鼠,雌雄各一只。在给药结束时,所有幸存的老鼠都被杀死。每组50只雄性小鼠,以两种剂量(5,000或10,000)中的一种注射2,4,6-三氯苯酚,持续105周。每组50只雌性老鼠被注射了两种剂量中的一种,最初是10,000或20,000 ppm,持续38周。由于给药组雌性的体重过度降低,雌性的剂量分别减少到2500 ppm和5000 ppm,并以较低剂量持续给药67周。雌性小鼠的时间加权平均剂量为5214或10428 ppm。配对的对照组由雌雄各20只未经治疗的老鼠组成。在给药结束时,所有幸存的老鼠都被杀死。在整个生物测定过程中,给药大鼠和小鼠的平均体重均低于相应的对照组,并与剂量相关。实验结束时,各组大鼠的存活率为68%或更高,各组小鼠的存活率为80%或更高。在雄性大鼠中,淋巴瘤或白血病的发生率与剂量相关(P=0.006),在直接比较中,低剂量组(P=0.019)和高剂量组(P=0.004)显著高于相应的对照组(对照4/20;低剂量的25/50;高剂量的29/50)。一些未患淋巴瘤或白血病的雄性大鼠也出现外周血白细胞增多、单核细胞增多和骨髓增生。在雌性大鼠中,单核细胞白血病的发生率并不显著。然而,与雄性大鼠一样,雌性大鼠出现外周血白细胞增多、单核细胞增多和骨髓增生,而对照组没有(血液白细胞增多和单核细胞增多:对照组0/20,低剂量6/50,高剂量3/50;骨髓增生:对照0/20,低剂量16/50,高剂量2/50)。在雄性和雌性小鼠中,肝细胞癌或腺瘤的发生率与剂量有关(P
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Bioassay of 2,4,6-trichlorophenol for possible carcinogenicity.

A bioassay of 2,4,6-trichlorophenol for possible carcinogenicity was conducted by administering the test chemical in feed to F344 rats and B6C3F1 mice. Groups of 50 rats of each sex were administered 2,4,6-trichlorophenol at one of two doses, either 5,000 or 10,000 ppm, for 106 or 107 weeks. Matched controls consisted of 20 untreated rats of each sex. All surviving rats were killed at the end of administration of the test chemical. Groups of 50 male mice were administered 2,4,6-trichlorophenol at one of two doses, either 5,000 or 10,000 for 105 weeks. Groups of 50 female mice were administered the test chemical at one of two doses, initially either 10,000 or 20,000 ppm, for 38 weeks. Because of excessively lowered body weights in the dosed groups of the females, the doses for the females were then reduced to 2,500 and 5,000 ppm, respectively, and administration at the lower doses was continued for 67 weeks. The time-weighted average doses for the female mice were either 5,214 or 10,428 ppm. Matched controls consisted of 20 untreated mice of each sex. All surviving mice were killed at the end of administration of the test chemical. Mean body weights of dosed rats and mice of each sex were lower than those of corresponding controls and were dose related throughout the bioassay. Survivals to the end of the experiment were 68% or greater in all groups of rats and 80% or greater in all groups of mice. In the male rats, lymphomas or leukemias occurred at incidences that were dose related (P=0.006) and in direct comparisons were significantly higher in the low-dose(P=0.019) and high-dose (P=0.004) groups than in the corresponding control group (controls 4/20; low-dose 25/50; high-dose 29/50). Leukocytosis and monocytosis of the peripheral blood and hyperplasia of the bone marrow also occurred in some dosed male rats not having lymphoma or leukemia. In female rats, monocytic leukemia did not occur at incidences that were significant. However, as in the male rats, leukocytosis and monocytosis of the peripheral blood and hyperplasia of the bone marrow occurred in the dosed female rats but not in the controls (blood leukocytosis and monocytosis: controls 0/20, low-dose 6/50, high-dose 3/50; bone marrow hyperplasia: controls 0/20, low-dose 16/50, high-dose 2/50). In both the male and female mice, hepatocellular carcinomas or adenomas occurred at incidences that were dose related (P<0.001), and in direct comparisons were significantly higher in the low- and high-dose male groups and the high-dose female group (P

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Bioassay of sulfisoxazole for possible carcinogenicity. Bioassay of diazinon for possible carcinogenicity. Bioassay of aldicarb for possible carcinogenicity. Bioassay of malaoxon for possible carcinogenicity. Bioassay of C.I. vat yellow 4 for possible carcinogenicity.
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