评估苯磺酸左旋氨氯地平化合物 I 对 SD 大鼠胚胎-胎儿发育的毒性和遗传毒性。

IF 3.3 4区 医学 Q2 REPRODUCTIVE BIOLOGY Reproductive toxicology Pub Date : 2024-07-31 DOI:10.1016/j.reprotox.2024.108676
Yijun Tian , Wenjing Shi , Fengjiang Liu , Huan Li , Tianbao Zhang , Yuping Zhu
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引用次数: 0

摘要

本研究采用胚胎-胎儿发育毒性试验评估了苯磺酸左旋氨氯地平对肥育斯普拉格-道利(SD)大鼠及其胚胎和同窝大鼠发育的影响。剂量为 20 毫克/千克时,观察到母体体重减轻,但在停止治疗后又恢复了。20 毫克/千克剂量组的胎鼠性别比例失调,雄性比例较高。虽然 20 毫克/千克剂量组对胎儿胸骨的发育有一定影响,但未观察到骨骼畸形。在 5 毫克/千克和 10 毫克/千克的剂量下,未发现母鼠(母体)有明显的大体形态异常,也未发现胎鼠有明显的胚胎毒性或胎儿毒性,胎鼠的身长和体重发育也未受到明显影响。遗传毒性的评估结合使用了阿姆斯试验、中国仓鼠卵巢细胞染色体畸变试验和 ICR 小鼠骨髓微核试验。阿姆斯试验结果表明,当剂量为 500 毫克/盘和 5000 毫克/盘时,具有很强的抑菌作用,当剂量为 0.5 毫克/盘、5 毫克/盘和 50 毫克/盘时,未观察到诱变性。剂量为 2.8、5.6 和 11.2 毫克/毫升时,对 CHO 细胞染色体畸变率无明显影响。在 ICR 小鼠微核试验中,各处理组的剂量分别为 3.125、6.25 和 12.5 毫克/千克时,均未观察到微核诱导效应。总之,在本实验条件下,苯磺酸左旋氨氯地平对肥育 SD 大鼠、其胚胎和仔鼠发育毒性的无观测不良效应水平(NOAEL)被确定为 10 毫克/千克/天。苯磺酸左旋氨氯地平没有表现出明显的遗传毒性。
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Evaluation of levamlodipine benzenesulfonate compound I for embryo-fetal developmental toxicity in SD rats and genotoxicity

In the present study, the effects of levamlodipine benzenesulfonate on the development of fertile Sprague-Dawley (SD) rats, their embryos, and littermates were assessed using an embryo-fetal developmental toxicity test. Maternal body weight reduction was observed at a dose of 20 mg/kg, but it recovered after treatment cessation. The 20 mg/kg dose group showed a skewed sex ratio in fetal rats, with a higher proportion of males. While some effects on fetal sternum development were observed at 20 mg/kg, no skeletal malformations were observed. No significant gross morphological abnormalities were detected in the dams (mothers), no significant embryotoxicity or foetotoxicity in fetal rats and no significant effects on fetal length and weight development at doses of 5 and 10 mg/kg. Genotoxicity was evaluated using a combination of the Ames test, the Chinese hamster ovary (CHO) cell chromosome aberration assay, and the ICR mouse bone marrow micronucleus test. The Ames test results indicated substantial bacteriostatic effects at doses of 500 and 5000 mg/dish, with no mutagenicity observed at doses of 0.5, 5, and 50 mg/dish. No significant effect on the aberration rate of CHO cell chromosomes was found at doses of 2.8, 5.6, and 11.2 mg/mL. In the ICR mouse micronucleus test, no micronucleus-inducing effect was observed at doses of 3.125, 6.25, and 12.5 mg/kg in each treatment group. In conclusion, under the conditions of this experiment, the no-observed-adverse-effect level (NOAEL) for developmental toxicity of levamlodipine benzenesulfonate in fertile SD rats, their embryos, and littermates was established to be 10 mg/kg/day. Levamlodipine benzenesulfonate did not exhibit significant genotoxicity.

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来源期刊
Reproductive toxicology
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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