Embryo-Fetal Developmental Toxicity Studies with Pregabalin in Mice and Rabbits

Dennis C. Morse
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引用次数: 14

Abstract

Pregabalin was evaluated for potential developmental toxicity in mice and rabbits. Pregabalin was administered once daily by oral gavage to female albino mice (500, 1250, or 2500 mg/kg) and New Zealand White rabbits (250, 500, or 1250 mg/kg) during organogenesis (gestation day 6 through 15 [mice] or 6 through 20 [rabbits]). Fetuses were evaluated for viability, growth, and morphological development. Pregabalin administration to mice did not induce maternal or developmental toxicity at doses up to 2500 mg/kg, which was associated with a maternal plasma exposure (AUC0–24) of 3790 μg•hr/ml, ≥30 times the expected human exposure at the maximum recommended daily dose (MRD; 600 mg/day). In rabbits, treatment-related clinical signs occurred at all doses (AUC0–24 of 1397, 2023, and 4803 μg•hr/ml at 250, 500, and 1250 mg/kg, respectively). Maternal toxicity was evident at all doses and included ataxia, hypoactivity, and cool to touch. In addition, abortion and females euthanized moribund with total resorption occurred at 1250 mg/kg. There were no treatment-related malformations at any dose. At 1250 mg/kg, compared with study and historical controls, the percentage of fetuses with retarded ossification was significantly increased and the mean number of ossification sites was decreased, which correlated with decreased fetal and placental weights, consistent with in utero growth retardation. Therefore, the no-effect dose for developmental toxicity in rabbits was 500 mg/kg, which produced systemic exposure approximately 16-times human exposure at the MRD. These findings indicate that pregabalin, at the highest dose tested, was not teratogenic in mice or rabbits

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普瑞巴林对小鼠和家兔的胚胎-胎儿发育毒性研究
评估普瑞巴林对小鼠和家兔的潜在发育毒性。在器官发生期间(妊娠第6 ~ 15天[小鼠]或妊娠第6 ~ 20天[兔]),雌性白化小鼠(500、1250或2500 mg/kg)和新西兰大白兔(250、500或1250 mg/kg)每天口服普瑞巴林1次。评估胎儿的生存能力、生长和形态发育。普瑞巴林给小鼠高达2500 mg/kg的剂量不会引起母体或发育毒性,这与母体血浆暴露(AUC0-24)为3790 μg•hr/ml有关,≥30倍于人类在最大推荐日剂量(MRD;600毫克/天)。家兔在所有剂量下均出现治疗相关临床症状(AUC0-24分别为1397、2023和4803 μg•hr/ml,剂量分别为250、500和1250 mg/kg)。母亲的毒性在所有剂量下都是明显的,包括共济失调、活动障碍和触摸时冰凉。总吸收量为1250 mg/kg时流产和死畜安乐死。在任何剂量下均无治疗相关畸形。在1250 mg/kg剂量下,与研究对照组和历史对照组相比,骨化迟缓的胎儿比例显著增加,平均骨化位点数量减少,这与胎儿和胎盘体重下降有关,与子宫内生长迟缓一致。因此,家兔发育毒性的无效应剂量为500 mg/kg,在MRD下产生的全身暴露量约为人类暴露量的16倍。这些发现表明,在测试的最高剂量下,普瑞巴林对小鼠或家兔没有致畸性
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来源期刊
CiteScore
1.65
自引率
0.00%
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0
审稿时长
>12 weeks
期刊介绍: The purpose of this journal is to publish original contributions describing the toxicity of chemicals to developing organisms and the process of reproduction. The scope of the journal will inlcude: • toxicity of new chemical entities and biotechnology derived products to developing organismal systems; • toxicity of these and other xenobiotic agents to reproductive function; • multi-generation studies; • endocrine-mediated toxicity, particularly for endpoints that are relevant to development and reproduction; • novel protocols for evaluating developmental and reproductive toxicity; Part B: Developmental and Reproductive Toxicology , formerly published as Teratogenesis, Carcinogenesis and Mutagenesis
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