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莫非佐辛(N - 22)的生殖与发育毒性研究(2)——大鼠胎儿器官形成期经口给予N - 22的研究

[Reproductive and developmental toxicity study of mofezolac (N-22) (2)--Study by oral administration of N-22 during the period of fetal organogenesis in rats].

作者信息

Toteno I, Haguro S, Furukawa S, Morinaga T, Morino K, Fujii S, Yamakita O

机构信息

Biological Research Center for the Protection of Environment, Shiga, Japan.

出版信息

J Toxicol Sci. 1990 Jun;15 Suppl 2:165-208. doi: 10.2131/jts.15.supplementii_165.

Abstract

The teratogenicity of mofezolac (N-22), a new developed analgesic and anti-inflammatory agent, was investigated in rats. N-22 was given orally to pregnant rats of the Jcl: Wistar strain (30 rats per group) at dose levels of 10, 50, 100 and 150 mg/kg/day from days 7 to 17 of gestation. Caesarean sections were performed on 20 dams per group on day 20 of gestation and their fetuses were examined for external, visceral and skeletal abnormalities. The remaining 10 dams per group were allowed to deliver and their offspring were examined for growth and reproductive performance. Results were as follows. 1. Effects on F0 generation At 150 mg/kg, eleven out of the 30 dams exhibited decreased motor activity, pale eyes, unkempt fur, urine-smeared lower abdomen, weakness and emaciation. At autopsy, twelve dams revealed gastrointestinal ulcers, peritonitic lesions, hypertrophy of the spleen, adrenal and mesenteric lymph node, atrophy of the submaxillary gland, thymus and liver and discoloration of the liver and kidney. Death, sacrificing in extremis, premature or delayed delivery and poor nursing occurred in one to two dams each. Food consumption was significantly decreased and body weight gain was significantly retarded in this dose level group. At 100 mg/kg, urine-smeared lower abdomen, hypertrophy of the spleen and poor nursing were observed in one dam each. 2. Effects on F1 generation At 150 mg/kg, significantly decreased fetal weight, increased number of immature fetuses and significantly retarded ossification of the 5th and 6th sternebrae and coccygeal vertebrae as well as significantly depressed body weight gain of female offspring were observed. No abnormalities were observed in each treated group in terms of development, behavior, learning ability and reproductive performance of offspring. 3. Effects on F2 generation No abnormalities were observed in fetuses and newborn young in each treated group. Based on these results, the maximum non-effective doses of N-22 in this study were considered to be 50 mg/kg/day for dams and offspring and 100 mg/kg/day for fetuses.

摘要

研究了新开发的镇痛抗炎药莫非唑酸(N - 22)对大鼠的致畸性。在妊娠第7天至第17天,将N - 22以10、50、100和150 mg/kg/天的剂量水平口服给予Jcl:Wistar品系的妊娠大鼠(每组30只)。在妊娠第20天,对每组20只母鼠进行剖腹产,并检查其胎儿的外部、内脏和骨骼异常。每组其余10只母鼠让其分娩,并检查其后代的生长和生殖性能。结果如下。1. 对F0代的影响 在150 mg/kg剂量下,30只母鼠中有11只表现出运动活动减少、眼睛苍白、皮毛凌乱、下腹有尿液痕迹、虚弱和消瘦。尸检时,12只母鼠出现胃肠道溃疡、腹膜炎病变、脾脏、肾上腺和肠系膜淋巴结肥大、颌下腺、胸腺和肝脏萎缩以及肝脏和肾脏变色。每组有1至2只母鼠出现死亡、濒死处死、早产或延迟分娩以及哺乳不良。该剂量水平组的食物消耗量显著降低,体重增加显著迟缓。在100 mg/kg剂量下,各有1只母鼠出现下腹有尿液痕迹、脾脏肥大和哺乳不良。2. 对F1代的影响 在150 mg/kg剂量下,观察到胎儿体重显著降低、未成熟胎儿数量增加、第5和第6胸骨节以及尾椎骨的骨化显著迟缓,以及雌性后代的体重增加显著受抑。在各治疗组中,后代的发育、行为、学习能力和生殖性能均未观察到异常。3. 对F2代的影响 各治疗组的胎儿和新生幼崽均未观察到异常。基于这些结果,本研究中N - 22对母鼠和后代的最大无作用剂量被认为是50 mg/kg/天,对胎儿是100 mg/kg/天。

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