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新型氟化果糖类似物作为己糖转运蛋白GLUT5的选择性探针。

New fluorinated fructose analogs as selective probes of the hexose transporter protein GLUT5.

作者信息

Soueidan Olivier-Mohamad, Trayner Brendan J, Grant Tina N, Henderson Jeff R, Wuest Frank, West F G, Cheeseman Chris I

机构信息

Department of Chemistry, 11227 Saskatchewan Drive University of Alberta, Edmonton, AB, Canada T6G 2G2.

出版信息

Org Biomol Chem. 2015 Jun 21;13(23):6511-21. doi: 10.1039/c5ob00314h. Epub 2015 May 15.

DOI:10.1039/c5ob00314h
PMID:25975431
Abstract

Facilitated hexose transporters (GLUTs) mediate the transport of hexoses and other substrates across the membranes of numerous cell types, and while some are expressed ubiquitously (e.g., GLUT1), others are more tissue specific (e.g., GLUT5). These properties have been exploited for the imaging of cancer cells by the use of hexose based probes, including fluorinated hexose derivatives for use with positron emission tomography (PET). However, design of new probes has been hampered by a limited understanding of how GLUT transporters interact with their substrates at the molecular level. Two fluorinated fructose surrogates designed for uptake by the GLUT5 transporter are described here: 3-deoxy-3-fluoro-D-fructose (3-FDF) and 1-deoxy-1-fluoro-2,5-anhydromannitol (1-FDAM). Synthesis (both cold and radiolabeled) and in vitro analysis of their transport characteristics in two breast cancer cell lines (EMT-6 and MCF-7) expressing GLUT5 are detailed. Both analogues are readily taken up into both cancer cell lines, with uptake mediated primarily by GLUT5. They also have low IC50 values, indicating a high affinity for the transporter, suggesting that the uptake of these probes would be unaffected by endogenously circulating fructose. Selective uptake by GLUT5 was also demonstrated in Xenopus oocytes. Finally, these results are the first demonstration that a hexose existing predominantly in the pyranose ring structure (3-FDF) is transported by GLUT5, strongly suggesting that this transporter can handle both furanose and pyranose forms of fructose.

摘要

易化型己糖转运蛋白(GLUTs)介导己糖和其他底物跨多种细胞类型的膜转运,虽然有些转运蛋白在全身广泛表达(如GLUT1),但其他的则具有更高的组织特异性(如GLUT5)。基于己糖的探针,包括用于正电子发射断层扫描(PET)的氟化己糖衍生物,已被用于癌细胞成像。然而,由于对GLUT转运蛋白如何在分子水平上与底物相互作用的了解有限,新探针的设计受到了阻碍。本文描述了两种设计用于被GLUT5转运蛋白摄取的氟化果糖替代物:3-脱氧-3-氟-D-果糖(3-FDF)和1-脱氧-1-氟-2,5-脱水甘露糖醇(1-FDAM)。详细介绍了它们(冷合成和放射性标记)的合成以及在两种表达GLUT5的乳腺癌细胞系(EMT-6和MCF-7)中的转运特性的体外分析。这两种类似物都很容易被两种癌细胞系摄取,摄取主要由GLUT5介导。它们还具有较低的IC50值,表明对转运蛋白具有高亲和力,这表明这些探针的摄取不会受到内源性循环果糖的影响。在非洲爪蟾卵母细胞中也证实了GLUT5的选择性摄取。最后,这些结果首次证明了主要以吡喃糖环结构存在的己糖(3-FDF)可被GLUT5转运,强烈表明该转运蛋白可以处理呋喃糖和吡喃糖形式的果糖。

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