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首页> 外文期刊>Frontiers in Chemistry >Ligand Screening Systems for Human Glucose Transporters as Tools in Drug Discovery
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Ligand Screening Systems for Human Glucose Transporters as Tools in Drug Discovery

机译:用于人类葡萄糖转运蛋白的配体筛选系统,作为药物发现中的工具

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摘要

Hexoses are the major source of energy and carbon skeletons for biosynthetic processes in all kingdoms of life. Their cellular uptake is mediated by specialized transporters, including glucose transporters (GLUT, SLC2 gene family). Malfunction or altered expression pattern of GLUTs in humans is associated with several widespread diseases including cancer, diabetes and severe metabolic disorders. Their high relevance in the medical area makes these transporters valuable drug targets and potential biomarkers. Nevertheless, the lack of a suitable high-throughput screening system has impeded the determination of compounds that would enable specific manipulation of GLUTs so far. Availability of structural data on several GLUTs enabled in silico ligand screening, though limited by the fact that only two major conformations of the transporters can be tested. Recently, convenient high-throughput microbial and cell-free screening systems have been developed. These remarkable achievements set the foundation for further and detailed elucidation of the molecular mechanisms of glucose transport and will also lead to great progress in the discovery of GLUT effectors as therapeutic agents. In this mini-review, we focus on recent efforts to identify potential GLUT-targeting drugs, based on a combination of structural biology and different assay systems.
机译:己糖是所有生命王国中生物合成过程的主要能量和碳骨架的来源。它们的细胞摄取由专门的转运蛋白介导,包括葡萄糖转运蛋白(GLUT,SLC2基因家族)。人中GLUT的功能异常或表达模式改变与多种广泛的疾病有关,包括癌症,糖尿病和严重的代谢紊乱。它们在医学领域的高度相关性使这些转运蛋白成为有价值的药物靶标和潜在的生物标志物。然而,缺乏合适的高通量筛选系统阻碍了迄今为止能够特异性操纵GLUT的化合物的确定。尽管受只能测试转运蛋白的两个主要构象的事实的限制,但几个GLUT上的结构数据的可用性实现了硅配体筛选。最近,已经开发了方便的高通量微生物和无细胞筛选系统。这些非凡的成就为进一步详细阐明葡萄糖转运的分子机制奠定了基础,并且还将在发现GLUT效应物作为治疗剂方面取得重大进展。在此小型审查中,我们将重点放在基于结构生物学和不同分析系统的组合基础上,以识别潜在的针对GLUT的药物的最新努力。

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