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氟在糖模拟药物设计中的作用。

The Role of Fluorine in Glycomimetic Drug Design.

机构信息

Department of Pharmaceutical Sciences, University of Basel, Pharmazentrum, Klingelbergstrasse 50, 4056, Basel, Switzerland.

出版信息

Chemistry. 2021 Feb 1;27(7):2240-2253. doi: 10.1002/chem.202003135. Epub 2020 Nov 26.

Abstract

Glycans are well established to play important roles at various stages of infection and disease, and ways to modulate these interactions have been sought as novel therapies. The use of native glycan structures has met with limited success, which can be attributed to their characteristic high polarity (e.g., low binding affinities) and inherently poor pharmacokinetic properties (e.g., short drug-target residence times, rapid renal excretion), leading to the development of 'glycomimetics'. Fluorinated drugs have become increasingly common over recent decades, with fluorinated glycomimetics offering some unique advantages. Deoxyfluorination maintains certain electrostatic interactions, while concomitantly reducing net polarity through 'polar hydrophobicity', improving residence times and binding affinities. Fluorination destabilizes the oxocarbenium transition state associated with metabolic degradation, and can restore exo- and endo-anomeric effects in C-glycosides and carbasugars. Lastly, it has shown great utility in radiotracer development and enhancement of antigenicity in glycan-based vaccines. Owing to synthetic challenges, fluorinated glycomimetics have been somewhat underutilized to date, but methodological improvements will advance their use in glycomimetic drugs.

摘要

糖链在感染和疾病的各个阶段都被证实起着重要作用,因此人们一直在寻找调节这些相互作用的方法,将其作为新型疗法。然而,使用天然糖链结构的方法收效甚微,这可以归因于其特征性的高极性(例如,低结合亲和力)和固有较差的药代动力学特性(例如,药物-靶标停留时间短,快速肾排泄),导致了“糖模拟物”的发展。在过去几十年中,氟化药物变得越来越普遍,氟化糖模拟物具有一些独特的优势。去氧氟化保持了某些静电相互作用,同时通过“极性疏水性”降低净极性,提高停留时间和结合亲和力。氟化还使与代谢降解相关的氧杂碳正离子过渡态不稳定,并可以恢复 C-糖苷和碳环糖中的外消旋和内消旋效应。最后,它在放射性示踪剂开发和糖基疫苗的抗原性增强方面显示出了巨大的应用潜力。由于合成方面的挑战,迄今为止,氟化糖模拟物的应用有些不足,但方法学的改进将促进其在糖模拟药物中的应用。

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