二霉素A类似物的构效关系:烷基对分子非脒端吡咯氮的影响,并结合下环的甲基消除。

L Grehn, U Ragnarsson, R Datema
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引用次数: 4

摘要

利用我们之前的策略合成了Distamycin A类似物5a-f (R = CnH2n+1, n = 0-5),并进行了一些改进修饰,筛选了它们对单纯疱疹病毒(HSV-1)的作用。病毒产量测定表明,5a-5d是有效的抗病毒药物,而5e和5f的活性较低。然而,在5a-5c中观察到相当大的细胞毒性。因此,结合显著抗病毒活性和适度细胞毒性的5d似乎是该系列中最有前途的衍生物。
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Structure-activity relationships in distamycin A analogues: effect of alkyl groups on the pyrrole nitrogen at the non-amidine end of the molecule combined with methyl elimination in the following ring.

Distamycin A analogues 5a-f (R = CnH2n+1, n = 0-5) were synthesized using our previous strategy with some improved modifications and screened for their effects on herpes simplex virus (HSV-1). Virus yield assays show that 5a-5d were potent antiviral agents whereas 5e and 5f had lower activity. Considerable cellular toxicity was however observed for 5a-5c. Thus 5d combining significant antiviral activity with moderate cellular toxicity seems to be the most promising derivative in this series.

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