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Phosphoramidates of 2'-beta-D-arabinouridine (AraU) as phosphate prodrugs; design, synthesis, in vitro activity and metabolism

机译:2'-β-D-阿拉伯糖尿苷(AraU)的磷酸酰胺盐,作为磷酸盐前药;设计,合成,体外活性和代谢

摘要

2'-Beta-D-arabinouridine (AraU), the uridine analogue of the anticancer agent AraC, was synthesized and evaluated for antiviral activity and cytotoxicity. In addition, a series of AraU monophosphate prodrugs in the form of triester phosphoramidates (ProTides) were also synthesized and tested against a range of viruses, leukaemia and solid tumour cell lines. Unfortunately, neither the parent compound (AraU) nor any of its ProTides showed antiviral activity, nor potent inhibitory activity against any of the cancer cell lines. Therefore, the metabolism of AraU phosphoramidates to release AraU monophosphate was investigated. The results showed carboxypeptidase Y, hog liver esterase and crude CEM tumor cell extracts to hydrolyse the ester motif of phosphoramidates with subsequent loss of the aryl group, while molecular modelling studies suggested that the AraU l-alanine aminoacyl phosphate derivative might not be a good substrate for the phosphoramidase enzyme Hint-1. These findings are in agreement with the observed disappearance of intact prodrug and concomitant appearance of the corresponding phosphoramidate intermediate derivative in CEM cell extracts without measurable formation of araU monophosphate. These findings may explain the poor antiviral/cytostatic potential of the prodrugs.
机译:合成了2'-β-D-阿拉伯尿苷(AraU),即抗癌剂AraC的尿苷类似物,并评估了其抗病毒活性和细胞毒性。此外,还合成了一系列三磷酸氨基磷酸酯(ProTides)形式的AraU单磷酸前药,并针对一系列病毒,白血病和实体瘤细胞系进行了测试。不幸的是,母体化合物(AraU)或其任何ProTides均未显示出抗病毒活性,也未显示出对任何癌细胞系的有效抑制活性。因此,研究了氨基磷酸AraU的代谢以释放单磷酸AraU。结果表明,羧肽酶Y,猪肝酯酶和粗制的CEM肿瘤细胞提取物可水解氨基磷酸酯的酯基序,随后失去芳基,而分子模型研究表明,AraU 1-丙氨酸氨酰基磷酸酯衍生物可能不是好的底物。用于磷酸酰胺酶Hint-1。这些发现与所观察到的完整前药的消失以及相应的氨基磷酸酯中间体衍生物在CEM细胞提取物中的伴随出现而没有可测量的araU单磷酸酯形成相一致。这些发现可能解释了前药的抗病毒/细胞抑制作用潜力不佳。

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