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氢氧化三苯基锡(万赛德KS)的急性和亚急性毒理学及安全性评价

Acute and subacute toxicology and safety evaluation of triphenyl tin hydroxide (Vancide KS).

作者信息

Winek C L, Marks M J, Shanor S P, Davis E R

出版信息

Clin Toxicol. 1978;13(2):281-96. doi: 10.3109/15563657808988238.

Abstract

The acute oral LD50 in Sprague-Dawley rats was determined to be 171 mg/kg (100-295) for males and 268 mg/kg (205-344) for females. 2. A 1 ppm dietary supplement of Vancide KS for 90 days did not induce any abnormalities in weanling Sprague-Dawley rats. The parameters evaluated were serum glutamic-oxaloacetic transaminase (SGOT), hematocrit, differential white blood cell count, food consumption, and weight gain, along with histologic studies of the myocardium, spleen, liver, kidney, stomach, and small intestine. A 500 ppm diet was lethal. Weanling and older rats subjected to 1000 and 10,000 ppm diets died within 5 days. 3. Vancide KS induced no acute dermal toxicity, nor did it exhibit percutaneous absorption in New Zealand strain albino rabbits. 4. Vancide KS induced no chronic dermal toxicity in New Zealand strain albino rabbits. 5. Vancide KS was not shown to be teratogenic. It exhibited an antifertility action, especially in Sprague-Dawley rats dosed on day 1 through day 7 of timed-pregnancy. 6. Vancide KS was shown to be an eye irritant which induces corneal opacity. 7. Acute oral toxicity studies in Sprague-Dawley rats indicate that Vancide KS should be classified as a toxic substance as defined in the regulations under the Federal Hazardous Labeling Act. 8. The intravenous administration of 25 mg/kg of Vancide KS to New Zealand strain albino rabbits induced death preceded by topic convulsions. 9. Vancide KS did not induce skin sensitization in male adult guinea pigs.

摘要
  1. 经测定,Vancide KS对雄性斯普拉格 - 道利大鼠的急性经口半数致死剂量为171毫克/千克(100 - 295),对雌性大鼠为268毫克/千克(205 - 344)。2. 在断奶的斯普拉格 - 道利大鼠的90天饮食中添加1 ppm的Vancide KS未诱发任何异常。所评估的参数包括血清谷草转氨酶(SGOT)、血细胞比容、白细胞分类计数、食物消耗量和体重增加,以及对心肌、脾脏、肝脏、肾脏、胃和小肠的组织学研究。500 ppm的饮食具有致死性。接受1000 ppm和10000 ppm饮食的断奶大鼠和成年大鼠在5天内死亡。3. Vancide KS未诱发急性皮肤毒性,在新西兰白兔中也未表现出经皮吸收。4. Vancide KS在新西兰白兔中未诱发慢性皮肤毒性。5. Vancide KS未显示出致畸性。它表现出抗生育作用,特别是在定时妊娠第1天至第7天给药的斯普拉格 - 道利大鼠中。6. Vancide KS被证明是一种眼刺激物,可诱发角膜混浊。7. 对斯普拉格 - 道利大鼠的急性经口毒性研究表明,Vancide KS应按照《联邦危险标签法》规定的法规归类为有毒物质。8. 给新西兰白兔静脉注射25毫克/千克的Vancide KS会导致其在抽搐后死亡。9. Vancide KS在成年雄性豚鼠中未诱发皮肤致敏。

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