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Novel Azetidine-Containing TZT-1027 Analogues as Antitumor Agents

机译:新型含氮杂环丁烷的TZT-1027类似物作为抗肿瘤药

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A conformational restriction strategy was used to design and synthesize nine TZT-1027 analogues. 3-Aryl-azetidine moiety was used to replace phenylethyl group of TZT-1027 at the C-terminus. These analogues exhibited moderate to excellent antiproliferative activities, and the most potent compound 1a showed IC 50 values of 2.2 nM against A549 and 2.1 nM against HCT116 cell lines, respectively. However, 1a could not achieve effective inhibition at all the dose levels in the A549 xenograft model (up to 5 mg/kg, injection, once a day), which is only 16%–35% inhibition at the end of the experiment.
机译:构象限制策略用于设计和合成九种TZT-1027类似物。 3-芳基氮杂环丁烷部分用于在C端取代TZT-1027的苯乙基。这些类似物表现出中等至优异的抗增殖活性,最有效的化合物1a对A549的IC 50值为2.2 nM,对HCT116细胞系的IC 50值为2.1 nM。但是,在A549异种移植模型(最高5 mg / kg,每天注射一次)中,在所有剂量水平下1a都无法达到有效抑制,在实验结束时只有16%–35%的抑制。

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