Natl Toxicol Program Tech Rep Ser. 1993 Aug;384:1-348.
1,2,3-Trichloropropane is a colorless liquid used as a paint and varnish remover, solvent, and degreasing agent, and as a crosslinking agent in the synthesis of polysulfides and hexafluoropropylene. 1,2,3-Trichloropropane may be found as an impurity in certain nematocides and soil fumigants and as a contaminant of drinking and ground water. Studies on the toxic and carcinogenic effects of 1,2,3-trichloropropane were initiated because of the close structural relationship of this chemical to other short-chain halogenated compounds that were demonstrated to be carcinogenic in experimental animals, and because of the potential for human exposure. Toxicology and carcinogenicity studies were conducted by administering 1,2,3-trichloropropane (greater than 99% pure) in corn oil by gavage to groups of F344/N rats and B6C3FI mice for 17 weeks and 2 years. Genetic toxicology studies were conducted in Salmonella typhimurium strains, mouse lymphoma cells, and Chinese hamster ovary cells. 17-Week Studies: Groups of 20 male and 20 female rats received 1,2,3-trichloropropane in corn oil by gavage at doses of 8, 16, 32, 63, 125, or 250 mg/kg body weight 5 days per week for up to 17 weeks; 30 male and 30 female rats received corn oil alone and served as controls. Animals were evaluated at 8 or 17 weeks. All rats in the 250 mg/kg groups died by week 5. One male and four female rats in the 125 mg/kg groups died during the study. The mean body weight gains and final mean body weights of males receiving 63 mg/kg and of males and females receiving 125 mg/kg were lower than those of the controls. Hematocrit values, hemoglobin concentrations, and erythrocyte counts decreased with dose in males and females. Serum alanine aminotransferase, aspartate aminotransferase, and sorbitol dehydrogenase activities were significantly increased in some female rats receiving 125 mg/kg. Serum pseudocholinesterase activity decreased with dose in females. Increases in kidney and liver weights were related to chemical administration. The principal toxic lesions associated with the administration of 1,2,3-trichloropropane to rats were hepatocellular necrosis, karyomegaly, and biliary hyperplasia of the liver; renal tubule necrosis, regeneration, and karyomegaly of the kidney; and necrosis and inflammation of the nasal olfactory and respiratory epithelium. Groups of 20 male and 20 female mice received 1,2,3-trichloropropane in corn oil by gavage at doses of 8, 16, 32, 63, 125, or 250 mg/kg 5 days per week for up to 17 weeks; 30 male and 30 female mice received corn oil alone and served as controls. Sixteen male and seven female mice in the 250 mg/kg groups died by week 4. The final mean body weights and mean body weight gains of dosed mice were similar to those of the controls, except those of 250 mg/kg males, which were lower than those of controls. The principal toxic lesions associated with the administration of 1,2,3-trichloropropane were hepatocellular necrosis and karyomegaly of the liver; necrosis, regeneration, and hyperplasia of the bronchiolar epithelium in the lung; and acanthosis (hyperplasia) and hyperkeratosis of the forestomach epithelium. 2-Year Studies: Groups of 60 male and 60 female rats received 0, 3, 10, or 30 mg 1,2,3-trichloropropane/kg body weight in corn oil by gavage 5 days per week for up to 104 weeks. Selection of 30 mg/kg as the high dose in these studies was based on the following chemical-related effects in the 17-week studies: deaths and liver and kidney lesions at 125 and 250 mg/kg and reduced final mean body weights and mean body weight gains at 63 mg/kg or greater. Groups of 60 male and 60 female mice received 0, 6, 20, or 60 mg 1,2,3-trichloropropane/kg body weight in corn oil by gavage 5 days per week for up to 104 weeks. Selection of 60 mg/kg as the high dose was based on chemical-related deaths and lesions of the liver, lung, and forestomach at 125 and 250 mg/kg in the 17-week studies. 15-Month Interim Evaluations: Up to 10 rats and 10 mice from each dose group were evaluated at 15 months. Absolute and relative liver and kidned kidney weights of dosed rats were significantly greater than those of the controls. Chemical-related nonneoplastic lesions and neoplasms of the forestomach, oral mucosa, pancreas (males), kidney, mammary gland (females), preputial gland, and clitoral gland were observed in dosed rats. Chemical-related nonneoplastic lesions and neoplasms of the forestomach and liver (females) were observed in dosed mice. Survival and Body Weight in the 2-Year Studies: Survival of male and female rats receiving 10 or 30 mg/kg 1,2,3-trichloropropane was significantly lower than that of controls. Two-year survival rates of male rats were: control, 34/50; 3 mg/kg, 32/50; 10 mg/kg, 14/49; 30 mg/kg, 0/52; and of females were: 31/50, 30/49, 8/52, 0/52. At 30 mg/kg, survival was markedly reduced due to chemical-related neoplasms, and survivors were killed in weeks 67 (females) or 77 (males). Final mean body weights of 30 mg/kg rats were 13% lower for males and 12% lower for females than those of controls; mean body weights of 3 and 10 mg/kg rats were similar to controls. Survival rates of mice receiving 6, 20, or 60 mg/kg 1,2,3-trichloropropane were also significantly lower than those of controls. Two-year survival rates of male mice were: 42/52, 18/51, 0/54, 0/56; and of female mice were: 41/50, 13/50, 0/51, 0/55. Because of reduced survival at 20 and 60 mg/kg due to chemical-related neoplasms, survivors were killed in weeks 73 (60 mg/kg females), 79 (60 mg/kg males), or 89 (20 mg/kg males and females). Final mean body weights were 16% lower for 60 mg/kg males, 18~ lower for 60 mg/kg females, and 13% lower for 20 mg/kg males than those of controls. Final mean body weights of 6 mg/kg males and females and 20 mg/kg females were similar to controls. Neoplasms and Nonneoplastic Lesions in the 2-Year Studies: Administration of 1,2,3-trichloropropane to rats induced benign and malignant neoplasms of the oral mucosa (pharynx and tongue), forestomach, and preputial and clitoral glands in males and females; benign neoplasms of the exocrine pancreas and kidney in males, and malignant neoplasms of the mammary gland in females. The incidences of squamous cell papillomas and carcinomas of the oral mucosa were significantly increased in 10 and 30 mg/kg rats, while the incidences of squamous cell papillomas or carcinomas (combined) of the forestomach were significantly increased in all dosed groups. The incidence of pancreatic acinar adenoma was significantly increased in dosed males, but not in dosed females. Similarly, the incidence of adenoma of the kidney was significantly increased in 10 and 30 mg/kg male rats only. The incidences of adenoma or carcinoma (combined) of the preputial gland in 30 mg/kg males and of the clitoral gland in 10 and 30 mg/kg females (homologous organs) were significantly increased. The incidence of adenocarcinoma of the mammary gland was significantly increased in the 10 and 30 mg/kg females. The incidences of Zymbal's gland carcinomas were increased in 30 mg/kg males and females. Adenocarcinomas of the intestine occurred in small numbers of dosed rats and may have been chemical related. In mice, the incidence of squamous cell carcinoma of the oral mucosa was significantly increased only in 60 mg/kg females. In contrast, the incidences of squamous cell papilloma and carcinoma of the forestomach were significantly increased in all groups of dosed mice. The incidences of hepatocellular adenoma or carcinoma (combined) were significantly increased in all dosed groups of males and 60 mg/kg females. The incidences of harderian gland adenoma were significantly increased in 20 mg/kg males and in 60 mg/kg males and females. The incidences of uterine adenoma, adenocarcinoma, and stromal polyp were significantly increased in 60 mg/kg females. Genetic Toxicology: 1,2,3-Trichloropropane was mutagenic in vitro in the presence of S9 metabolic activation. At two laboratories, positive responses were obtained for mutagenicity in Salmonella typhimurium strains TA97, TA98, TA100, and TA1535 in the presence of S9; no mutagenic activity was observed in TA1537, with or without S9. 1,2,3-Trichloropropane induced trifluorothymidine resistance in L5178Y mouse lymphoma cells with, but not without, S9. In cultured Chinese hamster ovary cells, sister chromatid exchanges and chromosomal aberrations were induced by 1,2,3-trichloropropane; however, significant increases in the endpoints of both cytogenetic effects occurred only in the presence of S9. Conclusions: Under the conditions of these 2-year gavage studies, there was clear evidence of carcinogenic activity of 1,2,3-trichloropropane in male F344/N rats based on increased incidences of squamous cell papillomas and carcinomas of the oral mucosa and forestomach, adenomas of the pancreas and kidney, adenomas or carcinomas of the preputial gland, and carcinomas of the Zymbal's gland. Adenomatous polyps and adenocarcinomas of the intestine may have been related to chemical administration. There was clear evidence of carcinogenic activity of 1,2,3-trichloropropane in female F344/N rats based on increased incidences of squamous cell papillomas and carcinomas of the oral mucosa and forestomach, adenomas or carcinomas of the clitoral gland, adenocarcinomas of the mammary gland, and carcinomas of the Zymbal's gland. Adenocarcinomas of the intestine may have been related to chemical administration. There was clear evidence of carcinogenic activity of 1,2,3-trichloropropane in male B6C3F1 mice based on increased incidences of squamous cell papillomas and carcinomas of the forestomach, hepatocellular adenomas or carcinomas of the liver, and harderian gland adenomas. Squamous cell papillomas of the oral mucosa may have been related to chemical administration. There was clear evidence of carcinogenic activity of 1,2,3-trichloropropane in female B6C3F1, mice based on increased incidences of squamous cell carcinomas of the oral mucosa, squamous cell papillomas and carcinomas of the forestomach, hepatocellular adenomas or carcinomas of the liver, harderian gland adenomas, and uterine adenomas, adenocarcinomas, and stromal polyps. Nonneoplastic lesions associated with exposure to 1,2,3-trichloropropane included increased severity of nephropathy in male rats and increased incidences of basal cell and squamous hyperplasia of the forestomach, acinar hyperplasia of the pancreas, renal tubule hyperplasia, and preputial or clitoral gland hyperplasia in male and female rats. Increased incidences of squamous hyperplasia of the forestomach and eosinophilic foci in the liver in male and female mice were chemical related. Synonyms: Allyl trichloride, glycerol tnchlorohydrin, glyceryl tnchlorohydrin, trichlorohydrin
1,2,3 - 三氯丙烷是一种无色液体,用作油漆和清漆去除剂、溶剂、脱脂剂,以及在多硫化物和六氟丙烯合成中作为交联剂。1,2,3 - 三氯丙烷可能作为某些杀线虫剂和土壤熏蒸剂中的杂质,以及作为饮用水和地下水的污染物被发现。由于该化学物质与其他在实验动物中被证明具有致癌性的短链卤代化合物结构密切相关,并且由于人类有接触的可能性,因此启动了对1,2,3 - 三氯丙烷毒性和致癌作用的研究。通过将1,2,3 - 三氯丙烷(纯度大于99%)溶于玉米油中,经口灌胃给予F344/N大鼠和B6C3F1小鼠组,进行了17周和2年的毒理学和致癌性研究。在鼠伤寒沙门氏菌菌株、小鼠淋巴瘤细胞和中国仓鼠卵巢细胞中进行了遗传毒理学研究。
17周研究:每组20只雄性和20只雌性大鼠,每周5天,经口灌胃给予溶于玉米油中的1,2,3 - 三氯丙烷,剂量分别为8、16、32、63、125或250 mg/kg体重,持续17周;30只雄性和30只雌性大鼠仅给予玉米油作为对照。在第8周或第17周对动物进行评估。250 mg/kg组的所有大鼠在第5周时死亡。125 mg/kg组中有1只雄性和4只雌性大鼠在研究期间死亡。接受63 mg/kg的雄性大鼠以及接受125 mg/kg的雄性和雌性大鼠的平均体重增加量和最终平均体重均低于对照组。雄性和雌性大鼠的血细胞比容值、血红蛋白浓度和红细胞计数随剂量降低。一些接受125 mg/kg的雌性大鼠血清丙氨酸氨基转移酶、天冬氨酸氨基转移酶和山梨醇脱氢酶活性显著增加。雌性大鼠血清假性胆碱酯酶活性随剂量降低。肾脏和肝脏重量的增加与化学物质给药有关。给大鼠施用1,2,3 - 三氯丙烷相关的主要毒性病变为肝细胞坏死、核肿大以及肝脏的胆管增生;肾小管坏死、再生以及肾脏的核肿大;以及鼻嗅觉和呼吸道上皮的坏死和炎症。每组20只雄性和20只雌性小鼠,每周5天,经口灌胃给予溶于玉米油中的1,2,3 - 三氯丙烷,剂量分别为8、16、32、63、125或250 mg/kg,持续17周;30只雄性和30只雌性小鼠仅给予玉米油作为对照。250 mg/kg组中有16只雄性和7只雌性小鼠在第4周时死亡。除250 mg/kg雄性小鼠外,给药小鼠的最终平均体重和平均体重增加量与对照组相似,250 mg/kg雄性小鼠的体重低于对照组。给小鼠施用1,2,3 - 三氯丙烷相关的主要毒性病变为肝细胞坏死和核肿大;肺细支气管上皮的坏死、再生和增生;以及前胃上皮的棘皮症(增生)和角化过度。
2年研究:每组60只雄性和60只雌性大鼠,每周5天,经口灌胃给予溶于玉米油中的0、3、10或30 mg 1,2,3 - 三氯丙烷/kg体重,持续104周。在这些研究中选择30 mg/kg作为高剂量是基于17周研究中的以下与化学物质相关的影响:125和250 mg/kg时出现死亡以及肝脏和肾脏病变,63 mg/kg及以上时最终平均体重和平均体重增加量降低。每组60只雄性和60只雌性小鼠,每周5天,经口灌胃给予溶于玉米油中的0、6、20或60 mg 1,2,3 - 三氯丙烷/kg体重,持续104周。选择60 mg/kg作为高剂量是基于17周研究中125和250 mg/kg时与化学物质相关的肝脏、肺和前胃的死亡和病变情况。
15个月中期评估:在15个月时对每个剂量组多达10只大鼠和10只小鼠进行评估。给药大鼠的肝脏和肾脏的绝对和相对重量显著大于对照组。在给药大鼠中观察到与化学物质相关的前胃、口腔黏膜、胰腺(雄性)、肾脏、乳腺(雌性)、包皮腺和阴蒂腺的非肿瘤性病变和肿瘤。在给药小鼠中观察到与化学物质相关的前胃和肝脏(雌性)的非肿瘤性病变和肿瘤。
2年研究中的生存和体重:接受10或30 mg/kg 1,2,3 - 三氯丙烷的雄性和雌性大鼠的生存率显著低于对照组。雄性大鼠的两年生存率为:对照组,34/50;3 mg/kg,32/50;10 mg/kg,14/49;30 mg/kg,0/52;雌性大鼠的两年生存率为:31/50,30/49,8/52,0/52。在30 mg/kg时,由于与化学物质相关的肿瘤,生存率显著降低,雌性幸存者在第67周死亡,雄性幸存者在第77周死亡。30 mg/kg大鼠的最终平均体重,雄性比对照组低13%,雌性比对照组低12%;3和10 mg/kg大鼠的平均体重与对照组相似。接受6、20或60 mg/kg 1,2,3 - 三氯丙烷的小鼠的生存率也显著低于对照组。雄性小鼠的两年生存率为:42/52,18/51,0/54,0/56;雌性小鼠的两年生存率为:41/50,13/50,0/51,0/55。由于20和60 mg/kg时因与化学物质相关的肿瘤导致生存率降低,60 mg/kg雌性小鼠在第73周、60 mg/kg雄性小鼠在第79周、20 mg/kg雄性和雌性小鼠在第89周处死幸存者。60 mg/kg雄性小鼠的最终平均体重比对照组低16%,60 mg/kg雌性小鼠低18%,20 mg/kg雄性小鼠低13%。6 mg/kg雄性和雌性小鼠以及20 mg/kg雌性小鼠的最终平均体重与对照组相似。
2年研究中的肿瘤和非肿瘤性病变:给大鼠施用1,2,3 - 三氯丙烷可诱导雄性和雌性大鼠口腔黏膜(咽和舌)、前胃、包皮腺和阴蒂腺的良性和恶性肿瘤;雄性大鼠外分泌胰腺和肾脏的良性肿瘤,以及雌性大鼠乳腺的恶性肿瘤。10和30 mg/kg大鼠口腔黏膜鳞状细胞乳头瘤和癌的发生率显著增加,而所有给药组前胃鳞状细胞乳头瘤或癌(合并)的发生率显著增加。给药雄性大鼠胰腺腺泡腺瘤的发生率显著增加,但给药雌性大鼠未增加。同样,仅10和30 mg/kg雄性大鼠肾脏腺瘤的发生率显著增加。30 mg/kg雄性大鼠包皮腺腺瘤或癌(合并)以及10和30 mg/kg雌性大鼠阴蒂腺(同源器官)腺瘤或癌(合并)的发生率显著增加。10和30 mg/kg雌性大鼠乳腺腺癌的发生率显著增加。30 mg/kg雄性和雌性大鼠鼓室腺腺癌的发生率增加。少数给药大鼠发生小肠腺癌,可能与化学物质有关。在小鼠中,仅60 mg/kg雌性小鼠口腔黏膜鳞状细胞癌的发生率显著增加。相比之下,所有给药组小鼠前胃鳞状细胞乳头瘤和癌的发生率显著增加。所有给药组雄性小鼠和60 mg/kg雌性小鼠肝细胞腺瘤或癌(合并)的发生率显著增加。20 mg/kg雄性小鼠以及60 mg/kg雄性和雌性小鼠哈德氏腺腺瘤的发生率显著增加。60 mg/kg雌性小鼠子宫腺瘤、腺癌和间质息肉的发生率显著增加。
在有S9代谢活化存在的情况下,1,2,3 - 三氯丙烷在体外具有致突变性。在两个实验室中,在有S9存在的情况下,鼠伤寒沙门氏菌菌株TA97、TA98、TA100和TA1535对1,2,3 - 三氯丙烷的诱变性呈阳性反应;在有或无S9的情况下,TA1537均未观察到诱变活性。1,2,3 - 三氯丙烷在有S(而非无S)存在的情况下可诱导L5178Y小鼠淋巴瘤细胞产生三氟胸苷抗性。在培养的中国仓鼠卵巢细胞中,1,2,3 - 三氯丙烷可诱导姐妹染色单体交换和染色体畸变;然而,仅在有S9存在的情况下,两种细胞遗传学效应的终点才显著增加。
在这些为期2年的经口灌胃研究条件下,有明确证据表明1,2,3 - 三氯丙烷对雄性F344/N大鼠具有致癌活性,依据为口腔黏膜和前胃鳞状细胞乳头瘤和癌、胰腺和肾脏腺瘤、包皮腺腺瘤或癌以及鼓室腺癌的发生率增加。小肠腺瘤性息肉和腺癌可能与化学物质给药有关。有明确证据表明1,2,3 - 三氯丙烷对雌性F344/N大鼠具有致癌活性,依据为口腔黏膜和前胃鳞状细胞乳头瘤和癌、阴蒂腺腺瘤或癌、乳腺腺癌以及鼓室腺癌的发生率增加。小肠腺癌可能与化学物质给药有关。有明确证据表明1,2,3 - 三氯丙烷对雄性B6C3F1小鼠具有致癌活性,依据为前胃鳞状细胞乳头瘤和癌、肝脏肝细胞腺瘤或癌以及哈德氏腺腺瘤的发生率增加。口腔黏膜鳞状细胞乳头瘤可能与化学物质给药有关。有明确证据表明1,2,3 - 三氯丙烷对雌性B6C3F1小鼠具有致癌活性,依据为口腔黏膜鳞状细胞癌、前胃鳞状细胞乳头瘤和癌、肝脏肝细胞腺瘤或癌、哈德氏腺腺瘤以及子宫腺瘤、腺癌和间质息肉的发生率增加。与接触1,2,3 - 三氯丙烷相关的非肿瘤性病变包括雄性大鼠肾病严重程度增加,以及雄性和雌性大鼠前胃基底细胞和鳞状上皮增生、胰腺腺泡增生、肾小管增生以及包皮或阴蒂腺增生的发生率增加。雄性和雌性小鼠前胃鳞状上皮增生和肝脏嗜酸性病灶发生率增加与化学物质有关。
烯丙基三氯、甘油三氯醇、甘油三氯代醇、三氯代醇
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