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首页> 外文期刊>Bioorganic and Medicinal Chemistry >Diversity-oriented chemical modification of heparin: Identification of charge-reduced N-acyl heparin derivatives having increased selectivity for heparin-binding proteins
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Diversity-oriented chemical modification of heparin: Identification of charge-reduced N-acyl heparin derivatives having increased selectivity for heparin-binding proteins

机译:肝素的面向多样性的化学修饰:鉴定对肝素结合蛋白具有更高选择性的减少电荷的N-酰基肝素衍生物

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摘要

The diversity-oriented chemical modification of heparin is shown to afford charge-reduced heparin derivatives that possess increased selectivity for binding heparin-binding proteins. Variable N-desulfonation of heparin was employed to afford heparin fractions possessing varied levels of free amine. These N-desulfonated heparin fractions were selectively N-acylated with structurally diverse carboxylic acids using a parallel synthesis protocol to generate a library of 133 heparin-derived structures. Screening library members to compare affinity for heparin-binding proteins revealed unique heparin-derived structures possessing increased affinity and selectivity for individual heparin-binding proteins. Moreover, N-sulfo groups in heparin previously shown to be required for heparin to bind specific proteins have been replaced with structurally diverse non-anionic moieties to afford identification of charge-reduced heparin derivatives that bind these proteins with equivalent or increased affinity compared to unmodified heparin. The methods described here outline a process that we feel will be applicable to the systematic chemical modification of natural polyanionic polysaccharides and the preparation of synthetic oligosaccharides to identify charge-reduced high affinity ligands for heparin-binding proteins.
机译:肝素的多样性导向化学修饰显示可提供电荷减少的肝素衍生物,该衍生物具有增强的结合肝素结合蛋白的选择性。肝素的可变N-脱磺作用被用于提供具有不同水平的游离胺的肝素级分。使用并行合成规程,使用结构多样的羧酸将这些N-脱硫的肝素级分选择性地N-酰化,以生成133种肝素衍生的结构的文库。筛选文库成员以比较对肝素结合蛋白的亲和力,发现独特的肝素衍生结构对单个肝素结合蛋白具有更高的亲和力和选择性。此外,以前证明肝素结合特定蛋白所需的肝素中的N-磺基已被结构上多样化的非阴离子部分所取代,以鉴定与未修饰的结合蛋白具有等同或增加亲和力的电荷降低的肝素衍生物。肝素。本文所述方法概述了我们认为适用于天然聚阴离子多糖的系统化学修饰和合成寡糖制备的过程,以鉴定与肝素结合蛋白的电荷降低的高亲和力配体。

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