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Application of phosphoramidate pronucleotide technology to abacavir leads to a significant enhancement of antiviral potency

机译:氨基磷酸酯原核苷酸技术在阿巴卡韦中的应用显着提高了抗病毒效力

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We report the first application of pronucleotide (ProTide) technology to the antiviral agent abacavir (Ziagen), used for the treatment of HIV infection. The phenylmethoxyalaninyl phosphoramidate of abacavir was prepared in good yield in one step. Also prepared was the corresponding phosphoramidate of the guanine nucleoside analogue "carbovir". The antiviral profile of each of the parent nucleosides was compared to that of the phosphoramidate ProTides. A significant (28- to 60-fold) increase in anti-HIV potency was noted for the ProTide of abacavir but not for that of carbovir. These findings were in agreement with the markedly higher (ca. 37-fold) levels of carbovir triphosphate that are formed in CEM cells upon response to the abacavir ProTide compared with the parent abacavir compound. In contrast the anti-HBV potency of both abacavir and carbovir were improved (10- and 20-fold, respectively) by ProTide formation. As in CEM cells, the abacavir ProTide provided significantly enhanced carbovir triphosphate levels in HepG2 2.2.15 cells over that of the parent nucleoside. On the basis of these data, a series of phosphoramidate analogues with structural variation in the ester and amino acid regions were prepared and their antiviral profiles described. In addition, the pharmacokinetic disposition of the abacavir phenylethoxyalaninyl phosphoramidate was evaluated in Cynomolgus monkeys.
机译:我们报告了前核苷酸(ProTide)技术在抗病毒药物abacavir(Ziagen)中的首次应用,该药物用于治疗HIV感染。一步制备阿巴卡韦的苯基甲氧基丙氨酰氨基磷酸酯。还制备了鸟嘌呤核苷类似物“ carbovir”的相应的氨基磷酸酯。将每个亲本核苷的抗病毒谱与氨基磷酸酯ProTides的抗病毒谱进行比较。对于阿巴卡韦的ProTide,抗HIV效力显着提高(28至60倍),而对卡波韦则没有。这些发现与母体阿巴卡韦化合物相比,对阿巴卡韦ProTide的应答在CEM细胞中形成的卡波韦三磷酸水平明显更高(约37倍)。相反,通过ProTide的形成,阿巴卡韦和卡博韦的抗HBV效力都得到了提高(分别是10倍和20倍)。像在CEM细胞中一样,阿巴卡韦ProTide在HepG2 2.2.15细胞中提供的卡波韦三磷酸水平明显高于亲本核苷。根据这些数据,制备了一系列在酯和氨基酸区域具有结构变化的氨基磷酸酯类似物,并描述了其抗病毒谱。另外,在食蟹猴中评估了阿巴卡韦苯基乙氧基丙氨酰氨基磷酸酯的药代动力学处置。

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