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使用母体肝细胞共培养在植入后大鼠胚胎培养中对环磷酰胺进行生物转化。

Biotransformation of cyclophosphamide in post-implantation rat embryo culture using maternal hepatocytes in co-culture.

作者信息

Piersma A H, van Aerts L A, Verhoef A, Garbis-Berkvens J M, Robinson J E, Peereboom-Stegeman J H, Peters P W

机构信息

Unit of Teratology, Endocrinology and Perinatal Screening, National Institute for Public Health and Environmental Protection, The Netherlands.

出版信息

Pharmacol Toxicol. 1991 Jul;69(1):47-51. doi: 10.1111/j.1600-0773.1991.tb00408.x.

Abstract

The post-implantation rat embryo culture technique is employed to study embryotoxic effects of xenobiotic compounds in the absence of the maternal compartment. For compounds biotransformed in vivo the embryo culture technique must be adapted in order to mimick the in vivo effects. In the present study the possibility of co-culturing metabolically active maternal hepatocytes suspended in the standard culture system with rat serum as a medium was investigated. Cyclophosphamide (CP) was used as a model compound as it needs bioactivation to display embryotoxicity. Morphologic and histologic effects were studied. Neither hepatocytes nor CP alone affected embryo development, whereas in the presence of hepatocytes embryotoxicity was observed at 30 micrograms/ml CP. Embryotoxicity was decreased in the additional presence of metyrapone, a monoxygenase inhibitor. Hepatocyte suspensions prepared via slicing or perfusion of livers were equally effective. In conclusion, co-culture of embryos and suspended hepatocytes can be performed under optimal conditions for embryo development and in the presence of biotransforming activity.

摘要

采用植入后大鼠胚胎培养技术,在无母体因素的情况下研究外源化合物的胚胎毒性作用。对于在体内进行生物转化的化合物,必须对胚胎培养技术进行调整,以模拟体内效应。在本研究中,研究了将悬浮于以大鼠血清为培养基的标准培养系统中的代谢活跃的母体肝细胞进行共培养的可能性。环磷酰胺(CP)用作模型化合物,因为它需要生物活化才能显示胚胎毒性。研究了形态学和组织学效应。单独的肝细胞和CP均未影响胚胎发育,而在有肝细胞存在的情况下,在30微克/毫升CP时观察到胚胎毒性。在另外存在单加氧酶抑制剂甲吡酮的情况下,胚胎毒性降低。通过肝脏切片或灌注制备的肝细胞悬液同样有效。总之,胚胎与悬浮肝细胞的共培养可在有利于胚胎发育的最佳条件下进行,且存在生物转化活性。

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