[N-(氟二氯甲基硫)邻苯二酰亚胺对大鼠28天重复剂量毒性试验]。

Y Matsushima, M Tsuda, K Naito, M Saitoh, K Isama, Y Ikarashi, Y Kawasaki, J Momma, S Kitajima, M Kaniwa
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引用次数: 0

摘要

N-(氟二氯甲基硫)邻苯二酰亚胺作为一种抗霉抗菌剂已得到广泛应用。本研究对Slc:Wistar大鼠进行了28天重复剂量口服氟叶酸酯的毒性研究。采用28 d重复给药试验方法,对5周龄雄性、雌性大鼠,每组10只,分别按0 (1% CMC钠,对照)、20、80、320 mg/kg(体重)灌胃氟folpet。对照组和320 mg/kg组在末次给药后14 d进行恢复试验。与对照组相比,320 mg/kg组的雄性和雌性体重增加明显减少。在320 mg/kg组,20只雄性大鼠中有5只和20只雌性大鼠中有4只在治疗期间死于呼吸困难。320 mg/kg组雌鼠血清ChE水平降至对照组的50%,γ - gt呈剂量依赖性升高,但未给药14 d后恢复。肝脏未见与治疗相关的组织病理学改变。320 mg/kg组男女均出现肾脏重量增加和肾小管空泡化现象。当剂量大于80 mg/kg时,男性出现角化过度和胃上皮增生,女性大于20 mg/kg。对呼吸困难的大鼠进行了重复给药的补充研究,结果显示氟叶酸灌胃可引起鼻腔和鼻咽部上皮的严重急性毒性损伤。氟绒被证明具有细胞毒性。总之,在重复给药毒性研究中采用的实验条件下,没有发现氟叶酸的无观察效应水平(NOEL)。
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[Twenty-eight days repeated dose toxicity test of N-(fluorodichloromethylthio)phthalimide in rats].

N-(Fluorodichloromethylthio)phthalimide (Fluor-folpet) has been widely used as an anti-mold and anti-bacterial agent. In this study, 28 days repeated-dose oral toxicity study of fluor-folpet was carried out in Slc:Wistar rats. An oral toxicity study for fluor-folpet, the twenty-eight days test, repeated-dose, oral administration, was performed as follows: Five week-old rats, male and female, 10 rats, each/group, were treated with intragastric administration of fluor-folpet with a dose of 0 (1% Sodium CMC, control), 20, 80 and 320 mg/kg, body weight. Recovery test, for 14 days after the last treatment, was examined for the control and the 320 mg/kg groups. The 320 mg/kg groups, both males and females, showed significantly reduced their body-weight gain compared with the control group. In the 320 mg/kg group, five out of 20 male rats and four out of 20 female rats died from dyspnea during the treatment period. In the female rats in the 320 mg/kg group, serum ChE level was decreased to 50% of control level and gamma-GT was increased in a dose-dependent manner, but these serum levels recovered after 14 days non-treatment period. No histopathological change, relating to the treatment, in liver was observed. Increased weight of the kidney and vacuolation in renal tubules were found in both sexes of 320 mg/kg group. Hyperkeratosis and hyperplasia of the stomach epithelium were observed at the dose more than 80 mg/kg in male, and more than 20 mg/kg in female. A supplemental study, repeated-dose, oral administration in rats carried out to examine the dyspnea revealed that severe acute toxic damages in epithelium of nasal cavity and meatus nasopharyngeus were induced by intragastric administration of fluor-folpet. Fluor-folpet is shown to be cytotoxic. In conclusion, the no-observed-effect level (NOEL) for fluor-folpet was not found under the experimental conditions employed in this repeated-dose toxicity study.

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