NTP technical report on the toxicity studies of Hexachloro-1,3-butadiene in B6C3F1 Mice (Feed Studies) (CAS No. 87-68-3).

Toxicity report series Pub Date : 1991-01-01
Raymond S.H. Yang
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Abstract

Two-week and 13-week toxicity studies of hexachloro-1,3-butadiene incorporated in the diet were conducted in B6C3F1 mice. Groups of five mice of each sex received diets containing 0, 30, 100, 300, 1,000, or 3,000 ppm hexachloro-1,3-butadiene for 15 days. Toxic responses in the 2-week studies, primarily in the higher dose groups, included abnormal clinical signs (lethargy, hunched posture, rough hair coats, light sensitivity, and/or in coordination), deaths (all mice in the two highest dose groups died by day 7), body and organ weight depression, and gross and histopathologic changes. The most prevalent microscopic lesion, seen in all hexachloro-1,3-butadiene-dosed mice, was renal tubular cell necrosis and/or regeneration. Regeneration was seen in lower dose groups. In addition to kidney lesions, histopathologic changes were also seen in the liver (hepatocyte necrosis, cytoplasmic vacuolization), lymphoid tissues (lymph node necrosis, depletion), and testis (seminiferous tubule giant cells) of mice in the two highest dose groups which died during the first week of the studies. Thirteen-week studies were conducted in which groups of 10 mice per sex received 0,1, 3,10, 30, or 100 ppm hexachloro-1,3-butadiene in feed (corresponding to doses of 0, 0.1, 0.4, 1.5, 4.9, or 16.8 mg/kg per day for males and 0.2, 0.5, 1.8, 4.5, or 19.2 mg/kg per day for females). No compound-related clinical signs or deaths were observed. Compared with controls, body weight gain was reduced in males receiving 30 and 100 ppm (-49% and -56%, respectively) and females receiving 100 ppm (-47%). Kidney weights were reduced in the males receiving 30 and 100 ppm and females receiving 100 ppm. A compound-related increase in tubular cell regeneration in the renal cortex occurred in male and female mice. This lesion, characterized by a diffuse increase in basophilia of the tubular epithelial cytoplasm and an increase in the number of nuclei, increased in severity with increased dose. The motility of sperm from dosed mice was lower, though not dose related, than that from controls. Female mice were more susceptible to the toxicity of hexachloro-1,3-butadiene than male mice. Based on the histopathologic evaluations, the no-observed-adverse-effect level appeared to be 10 ppm for the male mice in this 13-week study; no such level was identified for the female mice. Synonyms: HCBD; hexachlorobutadiene; 1,1,2,3,4,4-hexachloro-1,3- butadiene; perchlorobutadiene; C 46; Dolen-Pur, (NOTE: These studies were supported in part by funds from the Comprehensive Environmental Response, Compensation, and Liability Act trust fund (Superfund) by an interagency agreement with the Agency for Toxic Substances and Disease Registry, U.S. Public Health Service.)

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国家毒理学规划关于六氯-1,3-丁二烯对B6C3F1小鼠毒性研究的技术报告(饲料研究)(CAS编号87-68-3)。
对B6C3F1小鼠进行了为期两周和13周的六氯-1,3-丁二烯毒性研究。每组5只雌雄老鼠分别接受含有0、30、100、300、1000或3000 ppm六氯-1,3-丁二烯的饮食,为期15天。在为期2周的研究中,毒性反应主要发生在高剂量组,包括异常临床症状(嗜睡、驼腰姿势、毛糙、光敏感和/或协调)、死亡(两个最高剂量组的所有小鼠在第7天死亡)、身体和器官重量下降以及大体和组织病理学改变。在所有六氯-1,3-丁二烯剂量小鼠中,最常见的显微镜病变是肾小管细胞坏死和/或再生。低剂量组出现再生。除肾脏病变外,在研究第一周死亡的两个最高剂量组小鼠的肝脏(肝细胞坏死,细胞质空泡化),淋巴组织(淋巴结坏死,耗竭)和睾丸(精小管巨细胞)也可见组织病理学改变。在为期13周的研究中,每性别10只小鼠每组接受0、1、3、10、30或100 ppm六氯-1,3-丁二烯饲料(对应于雄性每天0、0.1、0.4、1.5、4.9或16.8 mg/kg的剂量,雌性每天0.2、0.5、1.8、4.5或19.2 mg/kg的剂量)。未观察到与化合物相关的临床症状或死亡。与对照组相比,摄入30 ppm和100 ppm(分别为-49%和-56%)的男性体重增加减少,摄入100 ppm(-47%)的女性体重增加减少。男性接受30 ppm和100 ppm,女性接受100 ppm,肾脏重量减轻。在雄性和雌性小鼠中,肾皮质小管细胞再生的化合物相关增加。这种病变的特点是小管上皮细胞质嗜碱性弥漫性增加,细胞核数量增加,随着剂量的增加,严重程度增加。与对照组相比,服用了药物的小鼠精子活力较低,但与剂量无关。雌性小鼠比雄性小鼠更容易受到六氯-1,3-丁二烯的毒性影响。根据组织病理学评估,在这项为期13周的研究中,雄性小鼠的未观察到的不良反应水平似乎为10ppm;在雌性小鼠中没有发现这种水平。同义词:HCBD;六氯丁二烯;1、1、2、3、4、4-hexachloro-1, 3 -丁二烯;perchlorobutadiene;C 46;(注:这些研究的部分资金来自《综合环境反应、赔偿和责任法案》信托基金(超级基金),并与美国公共卫生服务局有毒物质和疾病登记处达成了机构间协议。)
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