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硫酸化非糖基化糖胺聚糖类似物作为用于各种病理的新型药物发现平台。

Sulfated Non-Saccharide Glycosaminoglycan Mimetics as Novel Drug Discovery Platform for Various Pathologies.

机构信息

Department of Medicinal Chemistry and Institute for Structural Biology, Drug Discovery and Development, Virginia Commonwealth University, Richmond, Virginia 23219, United States.

Division of Basic Pharmaceutical Sciences, College of Pharmacy, Xavier University of Louisiana, New Orleans, Louisiana 70125, United States.

出版信息

Curr Med Chem. 2020;27(21):3412-3447. doi: 10.2174/0929867325666181120101147.

Abstract

Glycosaminoglycans (GAGs) are very complex, natural anionic polysaccharides. They are polymers of repeating disaccharide units of uronic acid and hexosamine residues. Owing to their template-free, spatiotemporally-controlled, and enzyme-mediated biosyntheses, GAGs possess enormous polydispersity, heterogeneity, and structural diversity which often translate into multiple biological roles. It is well documented that GAGs contribute to physiological and pathological processes by binding to proteins including serine proteases, serpins, chemokines, growth factors, and microbial proteins. Despite advances in the GAG field, the GAG-protein interface remains largely unexploited by drug discovery programs. Thus, Non-Saccharide Glycosaminoglycan Mimetics (NSGMs) have been rationally developed as a novel class of sulfated molecules that modulate GAG-protein interface to promote various biological outcomes of substantial benefit to human health. In this review, we describe the chemical, biochemical, and pharmacological aspects of recently reported NSGMs and highlight their therapeutic potentials as structurally and mechanistically novel anti-coagulants, anti-cancer agents, anti-emphysema agents, and anti-viral agents. We also describe the challenges that complicate their advancement and describe ongoing efforts to overcome these challenges with the aim of advancing the novel platform of NSGMs to clinical use.

摘要

糖胺聚糖(GAGs)是非常复杂的天然阴离子多糖。它们是由糖醛酸和己糖胺残基重复二糖单位组成的聚合物。由于其无模板、时空控制和酶介导的生物合成,GAGs 具有巨大的多分散性、异质性和结构多样性,这常常转化为多种生物学作用。有充分的文献记载表明,GAGs 通过与包括丝氨酸蛋白酶、丝氨酸蛋白酶抑制剂、趋化因子、生长因子和微生物蛋白在内的蛋白质结合,参与生理和病理过程。尽管在 GAG 领域取得了进展,但 GAG-蛋白界面在药物发现计划中仍然很大程度上未被开发。因此,非糖基化糖胺聚糖类似物(NSGMs)被合理地开发为一类新型的硫酸化分子,它们调节 GAG-蛋白界面,以促进对人类健康具有重要益处的各种生物学结果。在这篇综述中,我们描述了最近报道的 NSGMs 的化学、生化和药理学方面,并强调了它们作为结构和机制新颖的抗凝血剂、抗癌剂、抗肺气肿剂和抗病毒剂的治疗潜力。我们还描述了使它们的进展复杂化的挑战,并描述了正在进行的努力,以克服这些挑战,目的是将 NSGMs 的新型平台推进到临床应用。

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