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醋酸环丙孕酮和甲羟孕酮在小鼠胚胎植入前和植入后阶段治疗的致畸作用。I.

Teratogenic effects of cyproterone acetate and medroxyprogesterone treatment during the pre- and postimplantation period of mouse embryos. I.

作者信息

Eibs H G, Spielmann H, Hägele M

出版信息

Teratology. 1982 Feb;25(1):27-36. doi: 10.1002/tera.1420250105.

Abstract

Pregnant mice were treated with a single subcutaneous injection of either cyproterone acetate (CA) or medroxyprogesterone acetate (MPA). In the first experiment the animals received 5-900 mg/kg of the hormone before implantation (day 2 of pregnancy). CA treatment on day 2 caused a dose-dependent decrease in fetal weight and a significant dose-dependent increase in the rates of cleft palate and urinary tract abnormalities. Exencephaly and heart abnormalities were also significantly more frequent, but this increase was not dose-dependent. MPA treatment on day 2 was followed by sporadic increases in dead and resorbed fetuses, a decrease in fetal weight and an increase in the rates of cleft palate, and malformed or abnormally developed fetuses. None of these effects, however, was dose-dependent. In the second experiment the mice were given one single injection (30 mg/kg) of CA or MPA on any one of days 1-12 of gestation. Treatment with CA on one day between days 1 and 12 revealed that the specific sensitivity for abnormalities of the urinary tract was on days 5 and 6, for the respiratory tract on days 8 and 9, and for cleft palate on days 10 and 11. Treatment with MPA on one day between days 1 and 12 only revealed a high rate of respiratory and urinary tract abnormalities on day 9. After treatment with MPA cleft palate was again significantly more frequent in all treated groups, however, days of peak sensitivity were not detected. The long half-life of CA (60 hours) explains the teratogenic effect of high doses of this progestin after treatment on day 2 and also the pattern of abnormal development found after treatment with a single dose of CA on one of the days between day 1 and day 12.

摘要

给怀孕小鼠皮下注射一次醋酸环丙孕酮(CA)或醋酸甲羟孕酮(MPA)。在第一个实验中,动物在着床前(妊娠第2天)接受5 - 900 mg/kg的激素。第2天给予CA治疗导致胎儿体重呈剂量依赖性下降,腭裂和泌尿系统异常发生率呈显著剂量依赖性增加。无脑儿和心脏异常也明显更频繁,但这种增加不是剂量依赖性的。第2天给予MPA治疗后,死胎和吸收胎偶有增加,胎儿体重下降,腭裂、畸形或发育异常胎儿的发生率增加。然而,这些影响均非剂量依赖性。在第二个实验中,在妊娠第1 - 12天的任何一天给小鼠单次注射(30 mg/kg)CA或MPA。在第1天至第12天之间的某一天用CA治疗显示,泌尿系统异常的特异性敏感性在第5天和第6天,呼吸道异常在第8天和第9天,腭裂在第10天和第11天。在第1天至第12天之间的某一天用MPA治疗仅显示第9天呼吸道和泌尿系统异常发生率较高。用MPA治疗后,所有治疗组的腭裂再次明显更频繁,然而,未检测到峰值敏感天数。CA的长半衰期(60小时)解释了第2天治疗后高剂量这种孕激素的致畸作用,也解释了在第1天至第12天之间的某一天单次注射CA后发现的异常发育模式。

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