Organic Chemistry, Department of Chemistry, Faculty of Mathematics, Informatics and Natural Sciences, Universität Hamburg, Martin-Luther-King-Platz 6, D-20146, Hamburg, Germany.
Laboratory of Virology and Chemotherapy, Department of Microbiology and Immunology and Transplantation, Rega Institute for Medical Research, KU Leuven, Herestraat 49, Leuven, B-3000, Belgium.
Adv Sci (Weinh). 2023 Dec;10(36):e2306021. doi: 10.1002/advs.202306021. Epub 2023 Oct 26.
Nucleoside analogs require three phosphorylation steps catalyzed by cellular kinases to give their triphosphorylated metabolites. Herein, the synthesis of two types of triphosphate prodrugs of different nucleoside analogs is disclosed. Triphosphates comprising: i) a γ-phosphate or γ-phosphonate bearing a bioreversible acyloxybenzyl group and a long alkyl group and ii) γ-dialkyl phosphate/phosphonate modified nucleoside triphosphate analogs. Almost selective conversion of the former TriPPPro-compounds into the corresponding γ-alkylated nucleoside triphosphate derivatives is demonstrated in CEM/0 cell extracts that proved to be stable toward further hydrolysis. The latter γ-dialkylated triphosphate derivatives lead to the slow formation of the corresponding NDPs. Both types of TriPPPro-compounds are highly potent in wild-type CEM/0 cells and more importantly, they exhibit even better activities against HIV-2 replication in CEM/TK cell cultures. A finding of major importance is that, in primer extension assays, γ-phosphate-modified-NTPs, γ-mono-alkylated-triphosphates, and NDPs prove to be substrates for HIV-RT but not for cellular DNA-polymerases α,γ.
核苷类似物需要细胞激酶催化的三个磷酸化步骤才能产生其三磷酸代谢物。本文公开了两种不同核苷类似物的三磷酸前药的合成。三磷酸酯包括:i)带有生物可逆的acyloxybenzyl 基团和长烷基基团的γ-磷酸或γ-膦酸酯,以及 ii)γ-二烷基磷酸/膦酸酯修饰的核苷三磷酸类似物。在 CEM/0 细胞提取物中,几乎选择性地将前一种 TriPPPro 化合物转化为相应的 γ-烷基化核苷三磷酸衍生物,证明其对进一步水解稳定。后者的γ-二烷基化三磷酸酯衍生物导致相应的 NDPs 的缓慢形成。这两种类型的 TriPPPro 化合物在野生型 CEM/0 细胞中具有很高的效力,更重要的是,它们在 CEM/TK 细胞培养物中对 HIV-2 复制具有更好的活性。一个重要的发现是,在引物延伸测定中,γ-磷酸化修饰的 NTP、γ-单烷基化三磷酸酯和 NDP 被证明是 HIV-RT 的底物,但不是细胞 DNA 聚合酶 α、γ 的底物。
