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联合青蒿琥酯和甲氟喹抗疟药对大鼠发育毒性的研究。

Study on the developmental toxicity of combined artesunate and mefloquine antimalarial drugs on rats.

机构信息

Department of Pharmacology, Federal University of Paraná, CEP 81531-990 Curitiba, PR, Brazil.

出版信息

Reprod Toxicol. 2012 Dec;34(4):658-64. doi: 10.1016/j.reprotox.2012.10.004. Epub 2012 Oct 13.

Abstract

Antimalarial drug combinations containing artemisinins (ACTs) have become first choice therapies for Plasmodium falciparum malaria. Data on safety of ACTs in pregnancy are limited and no previous study has been conducted on the developmental toxicity of artesunate-mefloquine combinations on the first trimester of gestation. To evaluate the developmental toxicity of an artesunate/mefloquine combination, pregnant rats were treated orally with artesunate (15 and 40 mg/kg bwt/day), mefloquine (30 and 80 mg/kg bwt/day) and artesunate/mefloquine (15/30 and 40/80 mg/kg bwt/day) on gestation days 9-11. Dams were C-sectioned on day 20, and their uteri and fetuses removed and examined for soft tissue and skeleton abnormalities. Artesunate increased embryolethality and the incidence of limb long bone malformations on the absence of overt maternal toxicity. Mefloquine (80 mg/kg bwt/day) was maternally toxic and enhanced fetal variations. Combination of artesunate and mefloquine did not enhance their toxicity compared to the toxicity observed after its separate administration. Embryotoxicity of artesunate was apparently attenuated when it is co-administered with mefloquine.

摘要

含青蒿素的抗疟药物组合(ACT)已成为治疗恶性疟原虫疟疾的首选疗法。关于妊娠期 ACT 安全性的数据有限,以前没有研究过青蒿琥酯-甲氟喹组合在妊娠早期对胎儿发育的毒性。为了评估青蒿琥酯-甲氟喹组合的发育毒性,妊娠大鼠在妊娠第 9-11 天经口给予青蒿琥酯(15 和 40mg/kg bwt/天)、甲氟喹(30 和 80mg/kg bwt/天)和青蒿琥酯-甲氟喹(15/30 和 40/80mg/kg bwt/天)。在妊娠第 20 天进行 C 剖检,取出子宫及其胎儿,检查软组织和骨骼畸形。青蒿琥酯在没有明显母体毒性的情况下增加胚胎致死率和肢体长骨畸形的发生率。甲氟喹(80mg/kg bwt/天)对母体有毒性,并增强了胎儿的变异。青蒿琥酯和甲氟喹联合使用并未比单独给药后观察到的毒性增强其毒性。当青蒿琥酯与甲氟喹联合使用时,其胚胎毒性明显减弱。

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