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基于 d-葡萄糖和 d-甘露糖的抗代谢物。第 4 部分:2-脱氧-d-葡萄糖前药的单和二乙酸酯的简便合成,作为潜在有用的抗代谢物。

d-Glucose- and d-mannose-based antimetabolites. Part 4: Facile synthesis of mono- and di-acetates of 2-deoxy-d-glucose prodrugs as potentially useful antimetabolites.

机构信息

Department of Experimental Therapeutics, The University of Texas MD Anderson Cancer Center, Houston, TX, 77030, USA.

Department of Experimental Therapeutics, The University of Texas MD Anderson Cancer Center, Houston, TX, 77030, USA; Lukasiewicz-Industrial Chemistry Institute, Rydygiera 8, 01-793, Warsaw, Poland.

出版信息

Carbohydr Res. 2023 Sep;531:108861. doi: 10.1016/j.carres.2023.108861. Epub 2023 Jun 7.

DOI:10.1016/j.carres.2023.108861
PMID:37356236
Abstract

2-Deoxy-d-glucose (2-DG), a compound known to interfere with d-glucose and d-mannose metabolism, has been tested as a potential anticancer and antiviral agent. Preclinical and clinical studies focused on 2-DG have highlighted several limitations related to 2-DG drug-like properties, such as poor pharmacokinetic properties. To overcome this problem, we proposed design and synthesis of novel 2-DG prodrugs that subsequently could be tested using a variety of biochemical and molecular methods. We narrowed here our focus to esters of 2-DG as potential prodrugs based on the hypothesis that ubiquitous esterases will regenerate 2-DG, leading to increased circulation time of drug and adequate organ and tumor penetration. Testing this hypothesis in vitro and, especially, in vivo requires significant amounts of respective pure mono- and previously unknown di-acetylated water-soluble derivatives of 2-DG. Development of their efficient and practical method of synthesis was imperative. We describe novel facile and scalable syntheses of seven selectively acetylated water-soluble derivatives of 2-DG and present a detailed H and C NMR analysis of all final products. X-ray diffraction analysis has been performed for compound WP1122 that was selected for detailed preclinical and subsequent clinical evaluation as potential anticancer or antiviral agent.

摘要

2-脱氧-D-葡萄糖(2-DG)是一种已知的干扰 D-葡萄糖和 D-甘露糖代谢的化合物,已被测试作为一种潜在的抗癌和抗病毒药物。针对 2-DG 的临床前和临床研究强调了与 2-DG 药物相似特性相关的几个限制,例如较差的药代动力学特性。为了克服这个问题,我们提出了设计和合成新型 2-DG 前药的方案,随后可以使用各种生化和分子方法进行测试。我们在这里将重点缩小到 2-DG 的酯类作为潜在的前药,基于这样的假设,即普遍存在的酯酶将再生 2-DG,从而延长药物的循环时间,并使药物在适当的器官和肿瘤中渗透。在体外,特别是在体内测试这一假设需要大量相应的纯单乙酰化和以前未知的二乙酰化水溶性 2-DG 衍生物。因此,开发它们的高效和实用的合成方法是至关重要的。我们描述了 7 种选择性乙酰化水溶性 2-DG 衍生物的新型简便和可扩展的合成方法,并对所有最终产物进行了详细的 H 和 C NMR 分析。对于 WP1122 化合物进行了 X 射线衍射分析,该化合物被选为潜在的抗癌或抗病毒药物进行详细的临床前和随后的临床评估。

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