Bioassay of tetrachlorvinphos for possible carcinogenicity.

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Abstract

A bioassay of technical-grade tetrachlorvinphos for possible carcinogenicity was conducted by administering the test chemical in feed to Osborne-Mendel rats and B6C3F1 mice. Groups of 50 rats of each sex were administered tetrachlorvinphos at one of two doses for 80 weeks, then observed for 31 additional weeks. Time-weighted average doses were either 4,250 or 8,500 ppm. Matched controls consisted of groups of 10 untreated rats of each sex; pooled controls, used for statistical evaluation, consisted of the matched controls combined with 45 untreated male and 45 untreated female rats from similar bioassays of four other test chemicals. All surviving rats were killed at 111 weeks. Groups of 50 mice of each sex were administered tetrachlorvinphos at one of two doses, either 8,000 or 16,000 ppm, for 80 weeks, then observed for 12 additional weeks. Matched controls consisted of groups of 10 untreated mice of each sex; pooled controls, used for statistical evaluation, consisted of the matched controls combined with 40 untreated male and 40 untreated female mice from similar bioassays of four other test chemicals. All surviving mice were killed at 90-92 weeks. The mean body weights of the treated rats and mice were generally lower than those of the matched controls; however, the mortality rate was affected adversely by tetrachlorvinphos only in the male rats. Survival of all groups of rats and mice was adequate for meaningful statistical analyses of the incidence of tumors, except for a matched-control group of female rats for which the survival was abnormally low. In rats, C-cell adenoma of the thyroid showed a significant dose-related trend in the females, using pooled controls (controls 1/46, low-dose 2/50, high-dose 7/46, P=0.013), and by direct comparison, an increased incidence in the high-dose group (P=0.027). High incidences of C-cell hyperplasia in treated males and females further indicated a chemical-related effect on proliferative lesions of the thyroid. Cortical adenoma of the adrenal also showed a significant dose-related trend in the females, using pooled controls (controls 0/50, low-dose 2/49, high-dose 5/50,P=0.017), and by direct comparison, an increased incidence in the high-dose group (P=0.022). Hemangioma of the spleen occurred in male rats at a significantly higher incidence in the low-dose group than in the pooled controls (controls 0/52, low-dose 4/48, P=0.049); however, neither the incidence in the high-dose group (0/47) nor the test result for dose-related trend was statistically significant. In mice, hepatocellular carcinoma in males showed a highly significant dose-related trend, using either matched controls (controls 0/9, low-dose 36/50, high-dose 40/50, P<0.001) or pooled controls (controls 5/49, P<0.001). This finding was supported by direct comparisons of low- and high-dose groups of males with matched- or pooled-control groups, which showed highly significant increases in incidences of the tumor in the treated groups in all instances (P<0.001). In females, the incidence of hepatocellular carcinoma was not significant; however, the incidence of neoplastic nodule was significantly higher in both the low- and high-dose groups than in the pooled controls (controls 1/48, low-dose 14/49, P<0.001; high-dose 9/47, P=0.007), using pooled controls for tests for both doses. Because of this higher incidence in the low-dose group than in the high-dose group, there was a significant departure from linear trend (P=0.006). Granulomatous lesions of the liver were found in high proportions in both treated rats and treated mice, but none were found in matched controls. It is concluded that under the conditions of this bioassay, the administration of technical-grade tetrachlorvinphos in Osborne-Mendel rats was associated with proliferative lesions of the C cells of the thyroid and cortical adenomas of the adrenal in females. In female B6C3F1 mice, the incidence of neoplastic nodule of the liver was associated with treatment, and in male mice tetrachlorvinphos was carcinogenic, causing hepatocellular carcinoma of the liver.

四氯磷可能致癌性的生物测定。
通过给奥斯本-孟德尔大鼠和B6C3F1小鼠喂食饲料中的试验化学品,对技术级四氯磷可能的致癌性进行了生物测定。每组50只大鼠,雌雄各别,按两种剂量中的一种给药80周,然后再观察31周。时间加权平均剂量为4250 ppm或8500 ppm。配对的对照组由每性别10只未经治疗的大鼠组成;用于统计评估的混合对照组由匹配的对照组与45只未经处理的雄性和45只未经处理的雌性大鼠组成,这些大鼠来自其他四种测试化学品的类似生物测定。111周时处死所有存活的大鼠。每组50只雌雄老鼠分别以两种剂量(8000或16000 ppm)中的一种注射四氯磷80周,然后再观察12周。配对的对照组由每性别10只未治疗的小鼠组成;用于统计评估的混合对照组由匹配的对照组与40只未经处理的雄性和40只未经处理的雌性小鼠组成,这些小鼠来自其他四种测试化学物质的类似生物测定。所有存活小鼠在90 ~ 92周处死。治疗组大鼠和小鼠的平均体重普遍低于对照组;然而,四氯磷仅对雄性大鼠的死亡率有不利影响。所有各组大鼠和小鼠的存活率都足以进行有意义的肿瘤发生率统计分析,除了匹配的对照组雌性大鼠的存活率异常低。在大鼠中,采用合并对照(对照组1/46,低剂量2/50,高剂量7/46,P=0.013),雌性大鼠甲状腺c细胞腺瘤表现出显著的剂量相关趋势,直接比较,高剂量组发病率增加(P=0.027)。在接受治疗的男性和女性中,c细胞增生的高发生率进一步表明,化学物质对甲状腺增生性病变有相关作用。合并对照组(对照组0/50,低剂量2/49,高剂量5/50,P=0.017),女性肾上腺皮质腺瘤也显示出显著的剂量相关趋势,直接比较,高剂量组发生率增加(P=0.022)。低剂量组雄性大鼠脾脏血管瘤的发生率显著高于合并对照组(对照组0/52,低剂量组4/48,P=0.049);然而,高剂量组发病率(0/47)和剂量相关趋势的检测结果均无统计学意义。在小鼠中,雄性肝细胞癌显示出高度显著的剂量相关趋势,使用匹配的对照组(对照组0/9,低剂量36/50,高剂量40/50,P
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