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作为抗HIV活性剂的酸稳定2'-氟嘌呤双脱氧核苷

Acid-stable 2'-fluoro purine dideoxynucleosides as active agents against HIV.

作者信息

Marquez V E, Tseng C K, Mitsuya H, Aoki S, Kelley J A, Ford H, Roth J S, Broder S, Johns D G, Driscoll J S

机构信息

Laboratory of Medicinal Chemistry, National Cancer Institute, NIH, Bethesda, Maryland 20892.

出版信息

J Med Chem. 1990 Mar;33(3):978-85. doi: 10.1021/jm00165a015.

Abstract

2',3'-Dideoxy purine nucleosides have anti-HIV activity in vitro and the inosine analogue is being clinically evaluated. The instability of these compounds toward acidic conditions complicates oral administration. The effect of the addition of a fluorine atom to the 2'-position was investigated by preparing the fluorine-containing 2'-erythro and 2'-threo isomers of ddA and the threo isomer of ddI. All fluorine-containing compounds were indefinitely stable to acidic conditions which completely decomposed ddI (1) and ddA (2) in minutes. While the fluorine-containing erythro isomer, 5, was inactive, the threo isomers, 2'-F-dd-ara-A (3) and 2'-F-dd-ara-I (4), were just as potent and active in protecting CD4+ ATH8 cells from the cytopathogenic effects of HIV-1 as the parent drugs. Exposure to pH 1 at 37 degrees C prior to testing destroyed the activity of ddA and ddI but left the anti-HIV properties of 3 and 4 unchanged. The fluorinated analogues also protected cells exposed to HIV-2 and inhibited gag gene product expression but not as effectively as the parent compounds. The fluorine-containing analogues appear to be somewhat more toxic in vitro to the antigen- and mitogen-driven proliferation of immunocompetent cells than their corresponding parent compounds.

摘要

2',3'-二脱氧嘌呤核苷在体外具有抗HIV活性,其中肌苷类似物正在进行临床评估。这些化合物在酸性条件下不稳定,这使得口服给药变得复杂。通过制备ddA的含氟2'-赤型和2'-苏型异构体以及ddI的苏型异构体,研究了在2'-位添加氟原子的效果。所有含氟化合物在酸性条件下无限期稳定,而酸性条件能在几分钟内完全分解ddI(1)和ddA(2)。虽然含氟赤型异构体5没有活性,但苏型异构体2'-F-dd-ara-A(3)和2'-F-dd-ara-I(4)在保护CD4+ ATH8细胞免受HIV-1细胞病变效应方面与母体药物一样有效且具有活性。在测试前于37℃暴露于pH 1会破坏ddA和ddI的活性,但3和4的抗HIV特性不变。氟化类似物也能保护暴露于HIV-2的细胞并抑制gag基因产物表达,但效果不如母体化合物。含氟类似物在体外对免疫活性细胞的抗原和丝裂原驱动的增殖似乎比其相应的母体化合物毒性稍大。

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