Embryo-fetal developmental toxicity of carbamazepine administered orally in wistar rat

IF 3.3 4区医学 Q2 REPRODUCTIVE BIOLOGY

Reproductive toxicology Pub Date : 2024-07-14 DOI:10.1016/j.reprotox.2024.108665

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Abstract

Carbamazepine is an anticonvulsant medication commonly used to treat epilepsy and other neurological disorders. The purpose of this study was to assess the impact of carbamazepine on prenatal development, including maternal-fetal, external, visceral, and skeletal toxicity. Additionally, the study aimed to investigate the effects of orally administered Carbamazepine at a lower dose range in Wistar rats. Pregnant female rats were randomly distributed into control (G1) group administered with distilled water orally (n=8), low dose (G2) group administered at 25 mg/kg, intermediate dose (G3) group at 50 mg/kg, and high dose (G4) group at 100 mg/kg through oral gavage from gestation day (GD) 5–19. Pregnant female rats were scheduled to necropsy on gestation day (GD) 20. During the evaluation, the uterus was observed for number of live or viable fetuses, dead fetuses, early resorptions, late resorptions, number of corpora lutea and the sex ratio (m/f) per litter. Further, fetuses were subjected to materno-fetal examination which included observation for placenta, amniotic fluid, and umbilical cord followed by external evaluation. Additionally, half of the fetuses were subjected to visceral, craniofacial evaluation and other half of the fetuses were subjected to skeletal evaluation by double staining method using Alcian Blue for cartilages and Alizarin Red S for bones. It was observed that there was a significant decrease in the rate of pregnancy in the intermediate dose (G3) group and in high dose (G4) group when compared with the control group. Moreover, treatment with the Carbamazepine caused significant increase in fetal malformations such as dilation of lateral and third ventricle in brain, in intermediate dose (G3) group and high dose (G4) group when compared with the control (G1) group, dilation of ureters in high dose (G4) group. Fetal skeletal malformations like bent and nodulated ribs were also observed in intermediate dose (G3) group. Existing research substantially supports the claim that carbamazepine can cause teratogenic effects and prenatal development toxicity even at a lower dose range.

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口服卡马西平对 Wistar 大鼠胚胎-胎儿发育的毒性

卡马西平是一种抗惊厥药物，常用于治疗癫痫和其他神经系统疾病。本研究的目的是评估卡马西平对产前发育的影响，包括母胎毒性、外部毒性、内脏毒性和骨骼毒性。此外，该研究还旨在调查口服较低剂量范围的卡马西平对 Wistar 大鼠的影响。将怀孕雌性大鼠随机分为对照组（G1）、低剂量组（G2）、中剂量组（G3）和高剂量组（G4），对照组大鼠口服蒸馏水（n=8），中剂量组大鼠口服卡马西平（G2），剂量为 25 毫克/千克，高剂量组大鼠口服卡马西平（G4），剂量为 100 毫克/千克。怀孕雌性大鼠在妊娠第 20 天进行尸检。在评估过程中，观察子宫的活胎或可存活胎儿数量、死胎、早期再妊娠、晚期再妊娠、黄体数量和每胎性别比（m/f）。此外，还对胎儿进行母胎检查，包括观察胎盘、羊水和脐带，然后进行外部评估。此外，一半胎儿接受了内脏和颅面评估，另一半胎儿则接受了骨骼评估，采用阿尔新蓝（Alcian Blue）和茜素红（Alizarin Red S）双重染色法对软骨和骨骼进行染色。结果发现，与对照组相比，中剂量组（G3）和高剂量组（G4）的妊娠率明显下降。此外，与对照组（G1）相比，中剂量（G3）组和高剂量（G4）组的卡马西平治疗会导致胎儿畸形，如侧脑室和第三脑室扩张，高剂量（G4）组的输尿管扩张。在中剂量（G3）组还观察到胎儿骨骼畸形，如肋骨弯曲和结节。现有研究充分证明，即使剂量较低，卡马西平也会产生致畸效应和产前发育毒性。

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来源期刊

Reproductive toxicology 生物-毒理学

CiteScore

6.50

自引率

3.00%

发文量

131

审稿时长

45 days

期刊介绍： Drawing from a large number of disciplines, Reproductive Toxicology publishes timely, original research on the influence of chemical and physical agents on reproduction. Written by and for obstetricians, pediatricians, embryologists, teratologists, geneticists, toxicologists, andrologists, and others interested in detecting potential reproductive hazards, the journal is a forum for communication among researchers and practitioners. Articles focus on the application of in vitro, animal and clinical research to the practice of clinical medicine. All aspects of reproduction are within the scope of Reproductive Toxicology, including the formation and maturation of male and female gametes, sexual function, the events surrounding the fusion of gametes and the development of the fertilized ovum, nourishment and transport of the conceptus within the genital tract, implantation, embryogenesis, intrauterine growth, placentation and placental function, parturition, lactation and neonatal survival. Adverse reproductive effects in males will be considered as significant as adverse effects occurring in females. To provide a balanced presentation of approaches, equal emphasis will be given to clinical and animal or in vitro work. Typical end points that will be studied by contributors include infertility, sexual dysfunction, spontaneous abortion, malformations, abnormal histogenesis, stillbirth, intrauterine growth retardation, prematurity, behavioral abnormalities, and perinatal mortality.

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