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凝集素模拟物的分子结构和治疗潜力。

Molecular architecture and therapeutic potential of lectin mimics.

机构信息

Synthetic Cellular Chemistry Laboratory, RIKEN Advanced Science Institute, Wako, Saitama, Japan.

出版信息

Adv Carbohydr Chem Biochem. 2012;68:1-58. doi: 10.1016/B978-0-12-396523-3.00002-6.

Abstract

Lectins are proteins of non-immune origin that bind specific carbohydrates without chemical modification. Coupled with the emerging biological and pathological significance of carbohydrates, lectins have become extensively used as research tools in glycobiology. However, lectin-based drug development has been impeded by high manufacturing costs, low chemical stability, and the potential risk of initiating an unfavorable immune response. As alternatives to lectins, non-protein small molecules having carbohydrate-binding properties (lectin mimics) are currently attracting a great deal of attention because of their ease of preparation and chemical modification. Lectin mimics of synthetic origin are divided roughly into two groups, boronic acid-dependent and boronic acid-independent lectin mimics. This article outlines their representative architectures and carbohydrate-binding properties, and discusses their therapeutic potential by reviewing recent attempts to develop antiviral and antimicrobial agents using their architectures. We also focus on the naturally occurring lectin mimics, pradimicins and benanomicins. They are the only class of non-protein natural products having a C-type lectin-like ability to recognize d-mannopyranosides in the presence of Ca(2+) ions. Their molecular basis of carbohydrate recognition and therapeutic potential are also discussed.

摘要

凝集素是一类非免疫来源的蛋白质,能够在不发生化学修饰的情况下特异性地结合碳水化合物。加上碳水化合物在生物学和病理学方面的新兴意义,凝集素已广泛地被用作糖生物学研究的工具。然而,由于生产成本高、化学稳定性低以及可能引发不利免疫反应的风险,基于凝集素的药物研发受到了阻碍。作为凝集素的替代品,具有碳水化合物结合特性的非蛋白小分子(凝集素模拟物)因其易于制备和化学修饰而受到广泛关注。合成来源的凝集素模拟物大致可分为两类,即依赖硼酸和不依赖硼酸的凝集素模拟物。本文概述了它们的代表性结构和碳水化合物结合特性,并通过综述利用这些结构开发抗病毒和抗菌药物的最新尝试,讨论了它们的治疗潜力。我们还重点介绍了天然存在的凝集素模拟物——普拉地米星和贝那米星。它们是唯一一类具有 C 型凝集素样能力的非蛋白天然产物,能够在 Ca(2+) 离子存在的情况下识别 d-甘露吡喃糖苷。我们还讨论了它们的碳水化合物识别的分子基础和治疗潜力。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/3d3d/7158359/b57f40093857/sch01-01-9780123965233.jpg

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