2,4-二氨基甲苯可能致癌性的生物测定。

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In male rats, fibromas of the subcutaneous tissue occurred at incidences that were dose related (P=0.004) and in direct comparisons were higher in the dosed groups (P</= 0.020) than in the control group (controls 0/20, low-dose 15/30, high-dose 19/50). In the mice, hepatocellular carcinomas occurred in the females at incidences that were dose related (P=0.002) and in direct comparisons were higher in dosed groups (P</= 0.007) than in the control group (controls 0/19, low-dose 13/47, high-dose 18/46). In addition, lymphomas occurred at a significant incidence (P<0.001) in the low-dose female mice (controls 2/19, low-dose 29/47, high-dose 11/46). No tumors occurred at significantly increased incidences in the dosed male mice. Under the conditions of this bioassay, 2,4-diaminotoluene was carcinogenic for F344 rats, inducing hepatocellular carcinomas or neoplastic nodules in both males and females and carcinomas or adenomas of the mammary gland in females. 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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2,4-二氨基甲苯进行了可能致癌性的生物测定。每组50只雌雄老鼠分别以两种剂量中的一种注射2,4-二氨基甲苯,初始剂量为125 ppm或250 ppm,持续40周。由于低剂量组和高剂量组的平均体重增加量过度下降,因此剂量分别减少到50 ppm和100 ppm。对低剂量组持续给予50ppm,持续63周,然后杀死这些组中存活的动物。给予100 ppm高剂量雄性和雌性的存活动物分别在39周和44周结束时因发病率而死亡。低剂量男性和女性的时间加权平均剂量为79 ppm,高剂量男性为176 ppm,持续79周,高剂量女性为171 ppm,持续84周。配对的对照组包括20只未治疗的大鼠,雌雄各一只。每组各50只雌雄老鼠,以两种剂量(100或200 ppm)中的一种注射2,4-二氨基甲苯,持续101周。配对的对照组由雌雄各20只未经治疗的老鼠组成。在给药结束后,幸存的老鼠被杀死。除低剂量雄性小鼠的平均体重仅略低于对照组外,给药雄性和雌性大鼠和小鼠的平均体重均低于相应的对照组,且与剂量有关。雄性和雌性小鼠的死亡率与剂量无关,但雄性和雌性大鼠的死亡率都与剂量有关。在给予2,4-二氨基甲苯的动物中,观察到存活率降低和肝肾毒性病变。在雄性和雌性大鼠中,肝细胞癌或肿瘤结节的发生率均与剂量相关(P=0.014)。在直接比较对照组和给药组肿瘤发病率时,高剂量组男性发病率P值为0.026(男性:对照组0/20,低剂量5/49,高剂量10/50;女性:控制0/20;低剂量0/50,高剂量6/49)。这些肿瘤在雄性和雌性大鼠中发生的重要性,在同一实验室中,剂量组中相关的非肿瘤性肝脏病变的发生率很高,而在历史对照的雄性或雌性F344大鼠中肝脏肿瘤的发生率很低,这一点得到了支持。此外,雌性大鼠发生乳腺癌或腺瘤的发生率与剂量相关(P=0.002),并且在直接比较中,剂量组较高(P=0.002)
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Bioassay of 2,4-diaminotoluene for possible carcinogenicity.

A bioassay of 2,4-diaminotoluene 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-diaminotoluene at one of two doses, initially either 125 or 250 ppm, for 40 weeks. Because of excessive depression in the amount of mean body weight gained in both low- and high-dose groups, doses were then reduced to 50 and 100 ppm, respectively. Administration of 50 ppm to the low-dose groups was continued for 63 weeks, and surviving animals in these groups were then killed. Surviving animals in the high-dose males and females administered 100 ppm were killed at the end of 39 and 44 weeks, respectively, due to morbidity. The time-weighted average dose was 79 ppm for the low-dose male and females for 103 weeks, 176 ppm for the high-dose males for 79 weeks, and 171 ppm for the high-dose females for 84 weeks. Matched controls consisted of 20 untreated rats of each sex. Groups of 50 mice of each sex were administered 2,4-diaminotoluene at one of two doses, either 100 or 200 ppm, for 101 weeks. Matched controls consisted of 20 untreated mice of each sex. Surviving mice were killed at the end of administration of the test chemical. Mean body weights of dosed male and female rats and mice were lower than those of corresponding controls and were dose related except for the low-dose male mice, for which mean body weights were only slightly lower than those of controls. Mortality was not dose related in either the male or female mice, but was dose related in both the male and female rats. Survival was decreased and lesions of hepatonephrotoxicity were observed in the animals administered the 2,4-diaminotoluene. In the rats, hepatocellular carcinomas or neoplastic nodules occurred at incidences that were dose related in both the males (P=0.014) and the females (P=0.008). In direct comparisons of incidences of the tumors in control and dosed groups, the incidence in the high-dose male group had a P value of 0.026 (males: controls 0/20, low-dose 5/49, high-dose 10/50; females: controls 0/20; low-dose 0/50, high-dose 6/49). The significance of the occurrence of these tumors in both the male and female rats was supported by the high incidences of associated nonneoplastic lesions of the liver in the dosed groups and by low incidences of liver tumors in historical-control male or female F344 rats at the same laboratory. In addition, carcinomas or adenomas of the mammary gland occurred in the female rats at incidences that were dose related (P=0.002) and in direct comparisons were higher in the dosed groups (P<0.001) than in the control group (control 1/20; low-dose 38/50, high-dose 41/50). In male rats, fibromas of the subcutaneous tissue occurred at incidences that were dose related (P=0.004) and in direct comparisons were higher in the dosed groups (P

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