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17-丁酸氢化可的松21-丙酸酯的毒性研究 -2. 大鼠皮下注射的亚急性毒性(作者译)

[Studies on toxicity of hydrocortisone 17-butyrate 21-propionate -2. Subacute toxicity in rats by subcutaneous administration (author's transl)].

作者信息

Tarumoto Y, Kimura M, Abe S, Kasai A, Noda K, Nakane S, Sasajima M, Ohzeki M

出版信息

J Toxicol Sci. 1981 Jul;6 Suppl:17-46. doi: 10.2131/jts.6.supplement_17.

Abstract

Subacute toxicity of hydrocortisone 17-butyrate 21-propionate (HBP), a new synthetic corticosteroid, was studied in rats, using betamethasone 17-valerate (BV) and hydrocortisone 17-butyrate (HB) as the reference drugs. HBP was subcutaneously injected to rats at the daily doses of 0.08, 0.4, 2.0, 10 and 50 mg/kg for 30 days. BV and HB were also administered at the daily doses of 0.08, 0.4 and 2.0 mg/kg. The recovery test was performed for 4 weeks after administration of HBP, BV and HB. The suppression of body weight gain by HBP was observed at the doses more than 0.08 mg/kg in male and more than 2.0 mg/kg in female rats. In addition, at the doses more than 0.4 mg/kg of HBP induced the dose-dependent symptoms such as decrease in the number of circulating white blood cells, lymphocyte counts and S-ALP level, increase in total cholesterol, GOT and GPT level of serum, and regressive changes in adrenals, lymphatic and hematopoietic tissues. There were fatal cases in rats given 50 mg/kg of HBP. These changes are considered to be common phenomena to other corticosteroids, and less toxic in female than male rats. Changes of symptoms caused by the administration of HBP 2.0 mg/kg were almost recovered after withdrawal. The toxicities of three corticosteroids were in the order of BV greater than HB greater than or equal to HBP in strength. As the result, maximum non-toxic dose of HBP was estimated to be 0.08 mg/kg in female and lower than that in male rats.

摘要

以戊酸倍他米松(BV)和丁酸氢化可的松(HB)作为参比药物,对一种新型合成皮质类固醇17 - 丁酸 - 21 - 丙酸氢化可的松(HBP)在大鼠中的亚急性毒性进行了研究。将HBP以每日0.08、0.4、2.0、10和50 mg/kg的剂量皮下注射给大鼠,持续30天。BV和HB也分别以每日0.08、0.4和2.0 mg/kg的剂量给药。在给予HBP、BV和HB后进行了4周的恢复试验。在雄性大鼠中,剂量超过0.08 mg/kg以及在雌性大鼠中剂量超过2.0 mg/kg时,观察到HBP对体重增加有抑制作用。此外,当HBP剂量超过0.4 mg/kg时,会引发剂量依赖性症状,如循环白细胞数量、淋巴细胞计数和S - ALP水平降低,血清总胆固醇、GOT和GPT水平升高,以及肾上腺、淋巴和造血组织的退行性变化。给予50 mg/kg HBP的大鼠出现了死亡病例。这些变化被认为是其他皮质类固醇的常见现象,并且在雌性大鼠中的毒性低于雄性大鼠。给予2.0 mg/kg HBP引起的症状变化在停药后几乎恢复。三种皮质类固醇的毒性强度顺序为BV大于HB大于或等于HBP。结果表明,HBP的最大无毒剂量估计在雌性大鼠中为0.08 mg/kg,低于雄性大鼠。

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