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胸苷单磷酸的环外双键异构体的化学酶合成。

Chemo-enzymatic synthesis of the exocyclic olefin isomer of thymidine monophosphate.

机构信息

Department of Chemistry, University of Iowa, Iowa City, IA 52242-1294, United States.

Department of Chemistry, University of Iowa, Iowa City, IA 52242-1294, United States.

出版信息

Bioorg Med Chem. 2018 May 15;26(9):2365-2371. doi: 10.1016/j.bmc.2018.03.032. Epub 2018 Mar 22.

Abstract

Exocyclic olefin variants of thymidylate (dTMP) recently have been proposed as reaction intermediates for the thymidyl biosynthesis enzymes found in many pathogenic organisms, yet synthetic reports on these materials are lacking. Here we report two strategies to prepare the exocyclic olefin isomer of dTMP, which is a putative reaction intermediate in pathogenic thymidylate biosynthesis and a novel nucleotide analog. Our most effective strategy involves preserving the existing glyosidic bond of thymidine and manipulating the base to generate the exocyclic methylene moiety. We also report a successful enzymatic deoxyribosylation of a non-aromatic nucleobase isomer of thymine, which provides an additional strategy to access nucleotide analogs with disrupted ring conjugation or with reduced heterocyclic bases. The strategies reported here are straightforward and extendable towards the synthesis of various pyrimidine nucleotide analogs, which could lead to compounds of value in studies of enzyme reaction mechanisms or serve as templates for rational drug design.

摘要

最近有人提出,胸苷酸(dTMP)的环外双键变体可能是许多病原体中胸苷酸生物合成酶的反应中间体,但这些材料的合成报道尚缺乏。在这里,我们报告了两种制备 dTMP 环外双键异构体的策略,该异构体是病原体胸苷酸生物合成中的一种假定反应中间体,也是一种新型核苷酸类似物。我们最有效的策略涉及保留胸苷的现有糖苷键,并通过操作碱基生成环外亚甲基部分。我们还报告了成功的非芳香碱基胸腺嘧啶异构体的酶去脱氧核糖基化,这为获得具有破坏的环共轭或减少杂环碱基的核苷酸类似物提供了另一种策略。这里报道的策略简单直接,并可扩展到各种嘧啶核苷酸类似物的合成,这可能导致在研究酶反应机制方面有价值的化合物,或作为合理药物设计的模板。

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