碲酸乙酯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小鼠喂饲料,对技术级碲酸乙酯进行了可能致癌性的生物测定。每组各50只雌雄大鼠,分别以两种剂量(雄性300或600 ppm,雌性150或300 ppm)中的一种注射碲酸乙酯,持续105周。配对的对照组包括20只未治疗的大鼠,雌雄各一只。105周时处死所有存活的大鼠。每组50只雌雄老鼠分别服用两种剂量的碲酸乙酯,最初剂量为2500 ppm或5000 ppm。由于给药的动物有毒性迹象,这些剂量分别减少到500 ppm和2000 ppm,雄性从第41周开始,雌性从第38周开始。减少的剂量对雄性维持66周;对于雌性,减少的剂量在3周后分别增加到2,000和5,000 ppm,并保持在这些水平66周。男性的时间加权平均剂量为1,255或3,132 ppm;对于雌性来说,是2132或4915 ppm。配对的对照组由雌雄各20只未经治疗的老鼠组成。所有存活的小鼠在106周时被杀死。在整个生物测定过程中,给药组大鼠或小鼠的平均体重低于相应的对照组。在大鼠或小鼠中没有其他临床症状与试验化学物质的施用明显相关。大鼠和小鼠的生存没有受到化学物质的影响,所有组中都有足够数量的小鼠有发展为晚期肿瘤的风险。在雄性大鼠中,间皮瘤的发生率与剂量相关(P=0.012);直接比较,各剂量组肿瘤发生率均不显著高于对照组(对照组0/20,低剂量2/49,高剂量8/50)。然而,本实验室的历史对照数据显示,雄性F344大鼠的发病率为12/416(2.9%),而本研究中雄性高剂量组的发病率为8/50(16%)。在雌性大鼠中,没有肿瘤发生的发生率与试验化学物质的施用有关。在雄性和雌性小鼠中,给药组都发生了眼睛泪腺(哈德氏腺)瘤,但在相应的对照组中没有发生(雄性:对照组0/17;低剂量16/46,高剂量10/49;女性:对照组0/20,低剂量6/50,高剂量5/49)。剂量组的发病率没有高到足以显示具有统计学意义的剂量相关趋势。而在给药组和对照组雄性小鼠的直接比较中,低剂量雄性小鼠的发病率有统计学意义(P=0.003)。在雌性小鼠中,给药组和对照组的直接比较表明,该肿瘤的发病率没有统计学意义。在本实验条件下,tellurac乙酯对F344大鼠和B6C3F1小鼠均无致癌作用。给药雄性大鼠的间皮瘤发病率和给药雌雄小鼠的泪腺(哈德氏腺)腺瘤发病率提供了有启发性的证据,但在生物测定的条件下,不足以确定tellurac乙酯对这些动物的致癌性。
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Bioassay of ethyl tellurac for possible carcinogenicity.

A bioassay of technical-grade ethyl tellurac for possible carcinogenicity was conducted by administering the preparation in feed to F344 rats and B6C3F1 mice. Groups of 50 rats of each sex were administered ethyl tellurac at one of two doses, either 300 or 600 ppm for the males and either 150 or 300 ppm for the females, for 105 weeks. Matched controls consisted of 20 untreated rats of each sex. All surviving rats were killed at 105 weeks. Groups of 50 mice of each sex were administered ethyl tellurac at one of two doses, initially either 2,500 or 5,000 ppm. Due to signs of toxicity in the dosed animals, these doses were reduced to 500 and 2,000 ppm, respectively, starting at week 41 for the males and at week 38 for the females. The reduced doses were maintained for 66 weeks for the males; for the females, the reduced doses were raised after 3 weeks to 2,000 and 5,000 ppm, respectively, and maintained at these levels for 66 weeks. The time-weighted average doses for the males were either 1,255 or 3,132 ppm; for the females, either 2,132 or 4,915 ppm. Matched controls consisted of 20 untreated mice of each sex. All surviving mice were killed at 106 weeks. Mean body weights of the dosed groups of rats or mice were lower than those of corresponding controls throughout most or all of the bioassay. No other clinical signs in the rats or mice were clearly related to administration of the test chemical. Survival of the rats and the mice was not affected by the chemical, and sufficient numbers of all groups were at risk for the development of late-appearing tumors. In the male rats, mesotheliomas occurred at incidences that were dose related (P=0.012); in direct comparisons, the incidences of the tumors in the individual dosed groups were not significantly higher than that in the control group (controls 0/20, low-dose 2/49, high-dose 8/50). However, the historical-control data at this laboratory indicate an incidence of 12/416 (2.9%) in male F344 rats compared with 8/50 (16%) in the male high-dose group in this study. In the female rats, no tumors occurred at incidences that were related to administration of the test chemical. In both male and female mice, adenomas of the lacrimal (harderian) gland of the eye occurred in the dosed groups, but not in the corresponding controls (males: controls 0/17; low-dose 16/46, high-dose 10/49; females: controls 0/20, low-dose 6/50, high-dose 5/49). The incidences in the dosed groups were not high enough to show statistically significant dose-related trends. However, in direct comparisons of dosed and control groups of male mice, the incidence was statistically significant in the low-dose males (P=0.003). In female mice, direct comparisons of dosed and control groups indicated that the incidence of this tumor was not statistically significant. It is concluded that under the conditions of this bioassay, ethyl tellurac was not carcinogenic for F344 rats or B6C3F1 mice of either sex. The incidence of mesotheliomas in dosed male rats and the incidence of adenomas of the lacrimal (harderian) gland of the eye in dosed mice of either sex provided evidence which was suggestive but under the conditions of the bioassay insufficient to establish the carcinogenicity of ethyl tellurac in these animals.

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