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Toxicology of toluene diisocyanate.

机译:甲苯二异氰酸酯的毒理学。

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摘要

In studies on animals, toluene diisocyanate (TDI) was a contact and respiratory sensitizer, was not toxic by the oral or dermal routes, but was irritating, and toxic by inhalation. The respiratory tract was the target in acute, subchronic, and chronic exposure studies. Typically, at concentrations of above 0.1 ppm (parts per million), clinical signs of nasal irritation were evident, and histopathological investigations revealed rhinitis and epithelial hyperplasia of nasal passages. With increasing concentration, effects were more severe; affected the larynx, trachea, and lung; and, eventually, affected body weight and survival. The carcinogenicity of TDI to rats and mice was investigated. By inhalation, there was no treatment-related increase in tumor incidence in either species at the highest concentration tested (0.15 ppm). Effects of TDI were seen as rhinitis in nasal turbinates of both species, and as reduced body weight gain in mice. Through oral administration of TDI dissolved in corn oil to ratsand mice (up to 120 mg/kg/day), increased incidence of a number of tumor types was seen. This route is of questionable relevance to occupational exposure. The dosing solutions were known to have degraded, and TDI would hydrolyze to diaminotoluene in the acidic stomach environment. Several in vitro tests for genotoxicity gave positive results, which can be ascribed to degradation of TDI by solvents. In properly conducted assays, in vivo TDI was negative for genotoxicity. In a two-generation reproduction study in rats, there were no effects on reproductive indices at the highest exposure concentration of 0.3 ppm TDI, which elicited toxicity in both generations. In a developmental toxicity study in rats, there was evidence of minimal fetotoxicity in the presence of maternal toxicity at 0.5 ppm, with no effects at 0.1 ppm. No treatment-related embryotoxicity or teratogenicity was observed.
机译:在动物研究中,甲苯二异氰酸酯(TDI)是一种接触和呼吸道敏化剂,经口服或皮肤途径无毒,但具有刺激性,经吸入有毒。呼吸道是急性,亚慢性和慢性暴露研究的目标。通常,在浓度高于0.1 ppm(百万分之几)时,明显会出现鼻腔刺激的临床体征,并且组织病理学研究显示鼻腔炎是鼻炎和上皮增生。随着浓度的增加,影响更加严重。影响喉,气管和肺;并最终影响体重和生存。研究了TDI对大鼠和小鼠的致癌性。通过吸入,在测试的最高浓度(0.15 ppm)下,两种物种的肿瘤发病率均没有与治疗相关的增加。 TDI的作用被视为两种物种鼻甲的鼻炎,以及小鼠体重增加的减少。通过将溶解在玉米油中的TDI口服给予大鼠和小鼠(最高120 mg / kg /天),发现多种肿瘤的发病率增加。这条路线与职业接触有关。已知给药溶液已降解,TDI在酸性胃环境中会水解成二氨基甲苯。几种体外遗传毒性试验给出了积极的结果,这可以归因于溶剂对TDI的降解。在正确进行的测定中,体内TDI对基因毒性为阴性。在大鼠的两代生殖研究中,在最高暴露浓度为0.3 ppm TDI的情况下,对生殖指数没有影响,这在两代中均引起毒性。在大鼠的发育毒性研究中,有证据表明在母体毒性为0.5 ppm时,胎儿毒性最小,而在0.1 ppm时无作用。没有观察到与治疗有关的胚胎毒性或致畸性。

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