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大鼠肝细胞原代培养中的红霉素毒性

Erythromycin toxicity in primary cultures of rat hepatocytes.

作者信息

Villa P, Bégué J M, Guillouzo A

出版信息

Xenobiotica. 1985 Aug-Sep;15(8-9):767-73. doi: 10.3109/00498258509047439.

Abstract

Cultured rat hepatocytes were used to study the toxicity of erythromycin base (EB), erythromycin estolate (EE) and a new fluorinated derivative, (8S)-8-fluoroerythromycin A (EF). EF was not cytotoxic after 18 h incubation at concentrations up to 8 X 10(-4) M and EE was much more toxic than EB at all concentrations studied. EE toxicity was greater in a serum-free medium and was not increased by induction of cytochrome P-450 with phenobarbitone. In hepatocytes co-cultured with rat-liver epithelial cells EE, but not EF, raised the cytochrome P-450 content and formed stable cytochrome P-450 complexes with about 40% of the haemoprotein. The lack of correlation between cytochrome P-450 content and cytotoxicity suggests that some of the parent erythromycin drugs and not their metabolites are the toxic entities.

摘要

培养的大鼠肝细胞被用于研究红霉素碱(EB)、无味红霉素(EE)和一种新的氟化衍生物(8S)-8-氟红霉素A(EF)的毒性。在浓度高达8×10⁻⁴ M的情况下孵育18小时后,EF没有细胞毒性,并且在所有研究浓度下,EE的毒性都比EB大得多。在无血清培养基中,EE的毒性更大,并且用苯巴比妥诱导细胞色素P-450不会增加其毒性。在与大鼠肝脏上皮细胞共培养的肝细胞中,EE(而非EF)提高了细胞色素P-450的含量,并与约40%的血红素蛋白形成稳定的细胞色素P-450复合物。细胞色素P-450含量与细胞毒性之间缺乏相关性表明,一些红霉素原药而非其代谢产物是有毒物质。

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