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环己二胺四乙酸(CDTA)对小鼠的发育毒性

Developmental toxicity of cyclohexanediaminetetraacetic acid (CDTA) in mice.

作者信息

Sánchez D J, Colomina M T, Domingo J L, Llobet J M, Corbella J

机构信息

Laboratory of Toxicology and Biochemistry, School of Medicine, Rovira i Virgili University, San Lorenzo, Reus, Spain.

出版信息

Res Commun Chem Pathol Pharmacol. 1994 Mar;83(3):329-40.

PMID:8008982
Abstract

Cyclohexanediaminetetraacetic acid (CDTA), an effective antagonist for the treatment of zinc, lead, and manganese poisoning was evaluated for maternal and developmental toxicity in pregnant Swiss mice. CDTA was given intraperitoneally on gestation days 6-15 at doses of 0, 270, 540, and 1080 mg/kg/day. On gestational day 18, the fetuses were examined for external, visceral, and skeletal malformations and variations. Treatment with CDTA at 1080 mg/kg/day resulted in a high level of maternal deaths, as well as less severe clinical signs (significant reduction in weight gain and food consumption). Increased resorptions, fetal deaths, and decreased number of live fetuses per litter were observed at 1080 mg/kg/day. Mean fetal body weights were also significantly decreased in this group. At 1080 mg/kg/day, CDTA caused external malformations, while the development of skeletal tissues was less affected. The no observable adverse effect level (NOAEL) for maternal and developmental toxicity of CDTA in mice was 540 mg/kg/day. Analyses of maternal and fetal tissues revealed only slight effects of CDTA on concentrations of calcium, magnesium, zinc, copper and iron. According to these results, the alterations in mineral metabolism should not be the major reason for CDTA-induced developmental toxicity.

摘要

环己二胺四乙酸(CDTA)是一种治疗锌、铅和锰中毒的有效拮抗剂,本研究评估了其对怀孕瑞士小鼠的母体毒性和发育毒性。在妊娠第6至15天,以0、270、540和1080mg/kg/天的剂量腹腔注射CDTA。在妊娠第18天,检查胎儿的外部、内脏和骨骼畸形及变异情况。1080mg/kg/天剂量的CDTA治疗导致了高水平的母体死亡,以及不太严重的临床症状(体重增加和食物消耗显著减少)。在1080mg/kg/天剂量下,观察到吸收率增加、胎儿死亡以及每窝活胎数量减少。该组胎儿的平均体重也显著降低。在1080mg/kg/天剂量下,CDTA导致了外部畸形,而骨骼组织的发育受影响较小。CDTA对小鼠母体和发育毒性的无观察到有害作用水平(NOAEL)为540mg/kg/天。对母体和胎儿组织的分析表明,CDTA对钙、镁、锌、铜和铁浓度的影响很小。根据这些结果,矿物质代谢的改变不应是CDTA诱导发育毒性的主要原因。

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