NTP technical report on the toxicity studies of Pentachlorobenzene in F344/N Rats and B6C3F1 Mice (Feed Studies) (CAS No. 608-93-5).

Toxicity report series Pub Date : 1991-01-01
M. McDonald
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Abstract

Toxicology studies were conducted by exposing groups of F344/N rats and B6C3F1 mice of each sex to pentachlorobenzene (99%percnt; pure) in feed for 15 days or 13 weeks. Exposure concentrations were 0, 100, 330, 1,000, 3,300, or 10,000 ppm pentachlorobenzene in the 15-day studies (five animals of each sex per group per species). All rats that received 10,000 ppm and all mice that received 3,300 or 10,000 ppm died. Of the exposed rats that survived to the end of the studies, males had an accumulation of abnormal hyaline droplets in the renal cortical epithelium and males and females had centrilobular hepatocellular hypertrophy. Chemical-related lesions were not observed in exposed mice. Exposure concentrations were 0, 33, 100, 330, 1,000, or 2,000 ppm pentachlorobenzene in the 13-week studies (10 animals of each sex per group per species). No compound-related deaths occurred. Body weights of exposed rats but not of mice were lower than those of controls. In male rats, dose-related histologic lesions included renal tubular epithelial hyaline droplet formation and medullary granular casts and mineralization. This spectrum of renal lesions in male rats is consistent with the entity described as "hydrocarbon or hyaline droplet nephropathy." Exacerbation of spontaneous nephropathy characterized by renal tubular cell regeneration and homogeneous intratubular protein casts was seen in rats of each sex. Urinary protein concentration was increased in male and female rats in the 1,000- and 2,000-ppm groups; this change was especially prominent in males. Urinary glucose concentration was increased in male rats in the 330- to 2,000-ppm groups and in female rats in the 1,000 and 2,000-ppm groups. Centrilobular hepatocellular hypertrophy was observed in exposed male and female rats. Unidentified yellow-brown pigment granules were present in hepatocytes and renal tubular epithelium in exposed animals of each sex but were more prominent in females. These granules possibly contained porphyrins. The only exposure-related histologic lesion in mice of either sex was centrilobular hepatocellular hypertrophy. Significant, but not dose-related, increases of liver porphyrin concentrations were observed in exposed male rats; female rats in the 2,000-ppm group also had increased liver porphyrin concentrations. Liver porphyrin concentrations were significantly increased in the 1,000- and 2,000-ppm groups of mice of each sex. Increased sorbitol dehydrogenase concentrations in exposed rats and mice of each sex were attributed to mild hepatocyte injury. Minimal thyroid follicular cell hypertrophy was also present in male and female rats in the 1,000 and 2,000-ppm groups. Free thyroxin and total thyroxin concentrations were significantly decreased in exposed male and female rats; these data indicate moderate hypothyroxinemia in exposed animals. Hematologic findings in exposed rats included decreased hematocrit, hemoglobin concentration, erythrocyte count (males), mean corpuscular hemoglobin, mean erythrocyte volume, and mean corpuscular hemoglobin concentration; these findings are consistent with a mild-to-moderate anemia that is microcytic (decreased mean cell volume), hypochromic (decreased mean corpuscular hemoglobin concentration, females), and poorly regenerative (slight-to-no change in reticulocyte counts). The no-observed effect levels (NOELs) for histologic lesions were 33 ppm for male rats and 330 ppm for female rats. The NOEL for histologic lesions in female mice was 100 ppm. An NOEL was not reached for male mice. Synonyms: 1,2,3,4,5-Pentachlorobenzene; quintochlorobenzene. (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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五氯苯对F344/N大鼠和B6C3F1小鼠毒性研究技术报告(饲料研究)(CAS No. 608-93-5)。
毒理学研究是通过将F344/N大鼠和B6C3F1小鼠各组暴露于五氯苯(99%;纯)饲料15天或13周。在为期15天的研究中,五氯苯的暴露浓度分别为0、100、330、1000、3300或10,000 ppm(每组每物种每性别5只动物)。所有接受一万ppm的老鼠和3300或一万ppm的老鼠都死亡了。在存活到研究结束的暴露大鼠中,雄性在肾皮质上皮中有异常透明液滴的积累,雄性和雌性都有小叶中心肝细胞肥大。在暴露的小鼠中未观察到化学相关病变。在为期13周的研究中,五氯苯暴露浓度分别为0、33、100、330、1000或2000 ppm(每组每物种每性别10只动物)。没有发生与化合物有关的死亡。暴露大鼠的体重低于对照组,而小鼠的体重不低于对照组。在雄性大鼠中,剂量相关的组织学病变包括肾小管上皮透明液滴形成和髓质颗粒铸型和矿化。雄性大鼠肾脏病变的频谱与描述为“碳氢化合物或透明液滴肾病”的实体一致。以肾小管细胞再生和均匀的小管内蛋白铸型为特征的自发性肾病加重在各性别大鼠中均可见。在1,000 ppm和2,000 ppm组中,雄性和雌性大鼠的尿蛋白浓度增加;这种变化在男性中尤为明显。在ppm浓度为330- 2000的雄性大鼠和ppm浓度为1000 - 2000的雌性大鼠的尿葡萄糖浓度都有所增加。暴露的雌雄大鼠均可见小叶中心肝细胞肥大。暴露的雌雄动物的肝细胞和肾小管上皮中均存在不明的黄褐色色素颗粒,但在雌性中更为突出。这些颗粒可能含有卟啉。在雌雄小鼠中,唯一与暴露相关的组织学病变是小叶中心肝细胞肥大。暴露的雄性大鼠肝脏卟啉浓度显著升高,但与剂量无关;在2000 ppm组中,雌性大鼠的肝卟啉浓度也有所增加。在每一种性别的小鼠中,肝卟啉浓度在1000 ppm和2000 ppm组中显著增加。山梨糖醇脱氢酶在暴露的大鼠和小鼠中的浓度升高归因于轻度肝细胞损伤。在1,000和2,000 ppm组中,雄性和雌性大鼠的甲状腺滤泡细胞也出现了轻微的肥大。雄性和雌性暴露大鼠游离甲状腺素和总甲状腺素浓度显著降低;这些数据表明暴露的动物存在中度甲状腺功能低下。暴露大鼠的血液学结果包括红细胞压积、血红蛋白浓度、红细胞计数(雄性)、平均红细胞血红蛋白、平均红细胞体积和平均红细胞血红蛋白浓度下降;这些结果与轻至中度贫血相一致,表现为小细胞性贫血(平均细胞体积减少)、低色素性贫血(女性平均红细胞血红蛋白浓度降低)和再生能力差(网状红细胞计数轻微至无变化)。对组织学病变的无观察效应水平(NOELs)雄性大鼠为33 ppm,雌性大鼠为330 ppm。雌性小鼠组织学病变的NOEL为100ppm。没有对雄性小鼠进行NOEL测试。同义词:1、2、3、4、5-Pentachlorobenzene;quintochlorobenzene。(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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