The synthesis, stability and biological activity of bis-intercalating bis-daunomycin hydrazones.

Drug design and delivery Pub Date : 1990-03-01
D R Phillips, B C Baguley, R T Brownlee, P Cacioli, C J Chandler, I Kyratzis, J A Reiss, P A Scourides
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Abstract

The synthesis of a series of bis-daunomycin hydrazones (5a-g)--all moderately stable at 37 degrees C, pH 6.8, with a half-life of approximately 30 h--is reported. Under a pulse exposure of 2 h they exhibited growth inhibition of mouse L1210 cells, and were 2-3 fold more active than daunomycin. Under continuous exposure growth inhibition conditions with human colon cell lines (HT-29 and HCT-8) they hydrolysed to daunomycin and a partially hydrolysed mono-derivative of daunomycin, and there was no apparent increase in activity over that of the parent anthracycline. Their rate of hydrolysis was observed to increase rapidly with decreasing pH.

双插层双道霉素腙的合成、稳定性和生物活性。
报道了一系列双道诺霉素腙(5a-g)的合成,这些腙在37℃、pH 6.8下都是中等稳定的,半衰期约为30小时。在脉冲暴露2小时下,它们表现出对小鼠L1210细胞的生长抑制作用,活性比道诺霉素高2-3倍。在持续暴露于人类结肠细胞系(HT-29和HCT-8)生长抑制条件下,它们水解为道诺霉素和部分水解的道诺霉素单衍生物,与母体蒽环类药物相比,活性没有明显增加。它们的水解速率随着pH的降低而迅速增加。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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