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沙利度胺衍生物对非人灵长类动物绢毛猴的胚胎毒性作用。IV. 微克/千克剂量的EM12对映体的致畸性。

Embryotoxic effects of thalidomide derivatives in the non-human primate callithrix jacchus. IV. Teratogenicity of micrograms/kg doses of the EM12 enantiomers.

作者信息

Heger W, Schmahl H J, Klug S, Felies A, Nau H, Merker H J, Neubert D

机构信息

Institut für Toxikologie und Embryopharmakologie, Universitätsklinikum Rudolf Virchow, Freie Universität Berlin, Germany.

出版信息

Teratog Carcinog Mutagen. 1994;14(3):115-22. doi: 10.1002/tcm.1770140303.

Abstract

The dose-response of the teratogenic potency of the thalidomide (Thd) derivative EM12 was evaluated in the common marmoset (Callithrix jacchus). The smallest daily dose found to be effective was 30 micrograms EM12/kg body wt. This is the lowest dose of a Thd derivative ever reported to induce severe skeletal abnormalities. Ten micrograms EM12/kg body wt may be considered the no-observed-adverse-effect-level (NOAEL) under the experimental conditions chosen. The teratogenic potencies of the two EM12 enantiomers were tested at 100 micrograms/kg body wt, the dose which just induces an almost 100% effect in the case of the racemate. The S(-)-EM12 was found to induce typical severe limb abnormalities such as amelia, phocomelia, and radius aplasia, and none of the exposed fetuses were devoid of skeletal defects. In contrast, only few and minor skeletal defects were observed after application of the R(+) enantiomer. Although a pronounced teratogenic potency of the R(+)-EM12 can now largely be excluded, these low-dose studies are not sufficient to completely rule out any teratogenic potential of this enantiomer, since racemisation to small amounts of the S(-) form may occur in vivo. Further studies with Thd derivatives which are unable to racemise are necessary to prove the assumed complete ineffectiveness of the R(+) enantiomers.

摘要

在普通狨猴(Callithrix jacchus)中评估了沙利度胺(Thd)衍生物EM12致畸效力的剂量反应。发现有效的最小日剂量为30微克EM12/千克体重。这是有报道的能诱导严重骨骼异常的Thd衍生物的最低剂量。在所选实验条件下,10微克EM12/千克体重可被视为未观察到不良反应水平(NOAEL)。以100微克/千克体重测试了两种EM12对映体的致畸效力,该剂量在消旋体情况下刚好能诱导几乎100%的效应。发现S(-)-EM12能诱导典型的严重肢体异常,如无肢、短肢和桡骨发育不全,且所有暴露胎儿均有骨骼缺陷。相比之下,应用R(+)-对映体后仅观察到少数轻微的骨骼缺陷。尽管现在很大程度上可以排除R(+)-EM12有明显的致畸效力,但这些低剂量研究不足以完全排除该对映体的任何致畸潜力,因为在体内可能会发生少量消旋转化为S(-)形式。需要对不能发生消旋的Thd衍生物进行进一步研究,以证实假定的R(+)对映体完全无效。

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