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1,1 - 二氯 - 1 - 氟乙烷(HCFC - 141b)的急性和亚慢性毒性

Acute and subchronic toxicity of 1,1-dichloro-1-fluoroethane (HCFC-141b).

作者信息

Brock W J, Trochimowicz H J, Millischer R J, Farr C, Kawano T, Rusch G M

机构信息

E.I. DuPont de Nemours & Co., Haskell Laboratory, Newark, DE 19714, USA.

出版信息

Food Chem Toxicol. 1995 Jun;33(6):483-90. doi: 10.1016/0278-6915(95)00008-p.

Abstract

The acute and subchronic toxicity of 1,1-dichloro-1-fluoroethane (HCFC-141b), a CFC alternative, was evaluated in several acute and subchronic studies to assist in establishing proper handling guides. Data from acute toxicity studies in rats and rabbits demonstrated that HCFC-141b has very low acute toxicity. HCFC-141b was not a skin irritant, but was a mild eye irritant, in rabbits and was not a skin sensitizer in guinea pigs. Skin application of HCFC-141b to rabbits at 2000 mg/kg body weight produced no adverse effects. Oral administration at 5000 mg/kg body weight did not cause any deaths or clinical signs of toxicity in rats. The 4-hr LC50 for HCFC-141b was about 62,000 ppm in rats. Repeated exposures of rats for 6 hr/day, 5 days/wk for up to 90 days at concentrations of 2000, 8000 or 20,000 ppm did not result in significant adverse effects. Minor, but dose-dependent, reductions in body weight were observed in male and female rats during the 90-day study. Decreased responsiveness was also observed in rats but only at 20,000 ppm. An increase in serum cholesterol or triglycerides was observed in male and female rats at 20,000 ppm, and in males at 8000 ppm. No specific organ pathology was noted in these subchronic inhalation studies. The no-observable-adverse-effect level (NOAEL) from these studies was 8000 ppm. Results from other studies demonstrate that HCFC-141b was not neurotoxic in rats. As with trichlorofluoroethane (CFC-11), a cardiac sensitization response to an intravenous epinephrine challenge occurred in dogs with HCFC-141b at 5000 ppm and higher concentrations in experimental screening studies.

摘要

作为一种氟氯化碳替代品,1,1 - 二氯 - 1 - 氟乙烷(HCFC - 141b)的急性和亚慢性毒性在多项急性和亚慢性研究中进行了评估,以协助制定适当的处理指南。大鼠和兔子急性毒性研究的数据表明,HCFC - 141b的急性毒性非常低。在兔子中,HCFC - 141b不是皮肤刺激物,但为轻度眼刺激物,在豚鼠中不是皮肤致敏剂。以2000mg/kg体重对兔子进行皮肤涂抹未产生不良影响。以5000mg/kg体重对大鼠进行口服给药未导致任何死亡或毒性临床症状。HCFC - 141b在大鼠中的4小时半数致死浓度(LC50)约为62,000ppm。大鼠每天暴露6小时、每周5天,以2000、8000或20,000ppm的浓度重复暴露长达90天,未产生显著不良影响。在90天研究期间,雄性和雌性大鼠体重出现轻微但与剂量相关的减轻。在大鼠中也观察到反应性降低,但仅在20,000ppm时出现。在20,000ppm时,雄性和雌性大鼠以及8000ppm时的雄性大鼠血清胆固醇或甘油三酯升高。在这些亚慢性吸入研究中未发现特定器官病理学变化。这些研究的无可见不良作用水平(NOAEL)为8000ppm。其他研究结果表明,HCFC - 141b对大鼠无神经毒性。与三氯氟乙烷(CFC - 11)一样,在实验筛选研究中,当HCFC - 141b浓度达到5000ppm及更高时,犬对静脉注射肾上腺素激发产生心脏致敏反应。

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