地塞米松(兽药)。

Food safety (Tokyo, Japan) Pub Date : 2018-09-28 eCollection Date: 2018-09-01 DOI:10.14252/foodsafetyfscj.2018005s
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引用次数: 0

摘要

日本食品安全委员会(FSCJ)主要利用粮农组织/世卫组织食品添加剂联合专家委员会(JECFA)和欧洲药品管理局(EMEA)的评估报告,对合成肾上腺皮质激素地塞米松(CAS No. 50-02-2)进行了风险评估。地塞米松的主要不良反应是在各种毒性研究中发现的白细胞计数(WBC)减少、胸腺和脾脏萎缩以及肾上腺重量下降。这些影响可归因于糖皮质激素的作用。FSCJ支持EMEA“地塞米松与已知致癌物缺乏结构相似性”的判断,认为该药物不太可能致癌。在大鼠发育毒性研究中观察到致畸性,对胎儿的无观察到不良反应水平(NOAEL)为10 μg/kg bw/day。在一项内分泌学研究中,在各种毒理学研究中观察到的最低剂量的效果是减少了大鼠的白细胞。本研究NOAEL为1μg/kg bw/day。JECFA和EMEA根据大鼠肝脏中酪氨酸转氨酶活性(TAT)的药理作用规定了可接受的每日摄入量(ADI)。然而,FSCJ认为这个终点不适合建立ADI,因为TAT对糖皮质激素的反应是一种生理反应,TAT变化与毒理学结果的关系尚不清楚。因此,FSCJ根据一项内分泌学研究中大鼠的NOAEL为1μg/kg bw/day,应用安全系数为100,将地塞米松的每日推荐摄入量定为0.01μg/kg bw/day。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Dexamethasone (Veterinary medicinal products).

Food Safety Commission of Japan (FSCJ) conducted a risk assessment of dexamethasone (CAS No. 50-02-2), a synthetic adrenocortical hormone, using mainly the evaluation reports from the Joint FAO/WHO Expert Committee on Food Additives (JECFA), and the European Medicines Agency (EMEA). Major adverse effects of dexamethasone were observed in the decrease in white blood cell count (WBC), atrophy of thymus and spleen as well as the decrease in adrenal weights, which were found in various toxicity studies. These effects are attributable to the glucocorticoid action. FSCJ supported the EMEA's judgment "dexamethasone lacks structural similarity with known carcinogens", and concluded that this drug is unlikely to be carcinogenic. Teratogenicity was observed in rats developmental toxicity studies and the no-observed-adverse-effect level (NOAEL) for fetus was 10 μg/kg bw/day. The effect observed at the lowest dose in various toxicological studies was decreased WBC in rats in an endocrinological study. The NOAEL in this study was 1μg/kg bw/day. JECFA and EMEA specified an acceptable daily intake (ADI) based on the pharmacological action, the induction of tyrosine aminotransferase activity (TAT), in rat liver. However FSCJ judged this endpoint is not appropriate to establish an ADI, because the increase of TAT in response to glucocorticoid was a physiological response, and the relationship of changes in TAT with the toxicological findings was obscure. Consequently, FSCJ specified the ADI for dexamethasone at 0.01μg/kg bw/day, based on NOAEL of 1μg/kg bw/day, which was obtained in rats in an endocrinological study, applying a safety factor of 100.

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