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类视黄醇的体外致畸性。

In-vitro teratogenicity of retinoids.

作者信息

Steele C E, Marlow R, Turton J, Hicks R M

出版信息

Br J Exp Pathol. 1987 Apr;68(2):215-23.

Abstract

Mid-gestation rat conceptuses were cultured for 48 h in serum containing the retinoids all-trans-retinoic acid (TRA), 13-cis-retinoic acid (13-CRA), etretinate (ETR), etretin or one of six retinamides at concentrations ranging from 0.5 to 400 micrograms/ml. TRA was toxic at a concentration of 0.5 microgram/ml. 13-CRA and etretin caused abnormal development at 1.0 microgram/ml. However, the six retinamides were less toxic and adverse developmental effects were only evident at concentrations of 50 or 100 micrograms/ml. ETR was without effect at 100 micrograms/ml, the highest dose level of this compound tested. In vivo, TRA, 13-CRA and ETR are highly teratogenic. In this culture system, TRA and 13-CRA caused abnormal development at very low concentrations but in contrast, ETR was non-toxic at 100 micrograms/ml. Therefore these findings indicate that in vivo, maternal pharmacokinetics, and bioactivation in particular, play a major role in inducing abnormal development. Cis/trans isomerization was not a major determinant of toxicity. However, there appeared to be a relationship between abnormal development and the actual or estimated pKa values of the 10 retinoids tested.

摘要

将妊娠中期大鼠胚胎在含有视黄酸类物质的血清中培养48小时,这些视黄酸类物质包括全反式视黄酸(TRA)、13-顺式视黄酸(13-CRA)、依曲替酯(ETR)、阿维A以及六种视黄酰胺中的一种,浓度范围为0.5至400微克/毫升。TRA在浓度为0.5微克/毫升时具有毒性。13-CRA和阿维A在浓度为1.0微克/毫升时会导致发育异常。然而,六种视黄酰胺的毒性较小,只有在浓度为50或100微克/毫升时才会出现明显的不良发育影响。ETR在100微克/毫升(该化合物测试的最高剂量水平)时没有效果。在体内,TRA、13-CRA和ETR具有高度致畸性。在这个培养系统中,TRA和13-CRA在非常低的浓度下就会导致发育异常,但相比之下,ETR在100微克/毫升时无毒。因此,这些发现表明,在体内,母体药代动力学,尤其是生物活化,在诱导发育异常中起主要作用。顺式/反式异构化不是毒性的主要决定因素。然而,在所测试的10种视黄酸类物质的异常发育与实际或估计的pKa值之间似乎存在某种关系。

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