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曲安奈德、曲安西龙和皮质醇对大鼠的比较致畸性

Comparative teratogenicity of triamcinolone acetonide, triamcinolone, and cortisol in the rat.

作者信息

Rowland J M, Hendrickx A G

出版信息

Teratog Carcinog Mutagen. 1983;3(4):313-9. doi: 10.1002/1520-6866(1990)3:4<313::aid-tcm1770030402>3.0.co;2-6.

Abstract

Pregnant rats were injected im with 0.5 mg/kg triamcinolone acetonide (TAC) on day 12, 13, or 14 of gestation and the fetuses were examined for cleft palate on day 20. All three TAC-treated groups showed an increased proportion of fetuses with cleft palate compared to an untreated control group. Only the group treated on day 13 showed a significant increase in the proportion of litters affected. This indicates that day 13 of gestation is the most sensitive day for cleft palate induction by TAC in the rat. Pregnant rats were then treated on day 13 of gestation with either TAC, triamcinolone (TA), or cortisol. TAC was 59 times as potent as TA in inducing cleft palate, with ED50 values of 1.1 mg/kg and 65 mg/kg respectively. Cortisol induced a significant increase in cleft palates at 500 mg/kg, but the efficacy of this compound was too low to calculate an ED50 and relative teratogenic potency value. Other developmental abnormalities including umbilical hernias, resorption, and fetal death resulted from TAC treatment. Fetal growth retardation was produced by all three compounds. The rank order of teratogenic potency was determined to be TAC greater than TA greater than cortisol.

摘要

在妊娠第12、13或14天,给怀孕大鼠腹腔注射0.5mg/kg曲安奈德(TAC),并在第20天检查胎儿是否腭裂。与未处理的对照组相比,所有三个TAC处理组腭裂胎儿的比例均增加。只有在第13天处理的组受影响窝数的比例显著增加。这表明妊娠第13天是大鼠中TAC诱导腭裂最敏感的一天。然后在妊娠第13天用TAC、曲安西龙(TA)或皮质醇处理怀孕大鼠。TAC诱导腭裂的效力是TA的59倍,ED50值分别为1.1mg/kg和65mg/kg。皮质醇在500mg/kg时诱导腭裂显著增加,但该化合物的效力太低,无法计算ED50和相对致畸效力值。TAC处理导致其他发育异常,包括脐疝、吸收和胎儿死亡。所有三种化合物均导致胎儿生长迟缓。致畸效力的顺序确定为TAC大于TA大于皮质醇。

相似文献

1
Comparative teratogenicity of triamcinolone acetonide, triamcinolone, and cortisol in the rat.曲安奈德、曲安西龙和皮质醇对大鼠的比较致畸性
Teratog Carcinog Mutagen. 1983;3(4):313-9. doi: 10.1002/1520-6866(1990)3:4<313::aid-tcm1770030402>3.0.co;2-6.
2
Teratogenicity of triamcinolone acetonide in rats.
Teratology. 1983 Feb;27(1):13-8. doi: 10.1002/tera.1420270104.

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