Establishing a yeast-based screening system for discovery of human GLUT5 inhibitors and activators

Human GLUT5 is a fructose-specific transporter in the glucose transporter family (GLUT, SLC2 gene family). Its substrate-specificity and tissue-specific expression make it a promising target for treatment of diabetes, metabolic syndrome and cancer, but few GLUT5 inhibitors are known. To identify and...

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Published inScientific reports Vol. 7; no. 1; pp. 6197 - 9
Main Authors Tripp, Joanna, Essl, Christine, Iancu, Cristina V., Boles, Eckhard, Choe, Jun-yong, Oreb, Mislav
Format Journal Article
LanguageEnglish
Published London Nature Publishing Group UK 24.07.2017
Nature Publishing Group
Nature Portfolio
Subjects
14
14/19
631/154/1435/2163
631/45/72/1204
Cancer
Diabetes mellitus
Epicatechin
Fructose
Glucose transporter
Glucose transporter type 5
High-throughput screening
Humanities and Social Sciences
Inhibitors
Ligands
Metabolic disorders
Metabolic syndrome
multidisciplinary
Science
Science (multidisciplinary)
Yeast
Yeasts
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Summary:Human GLUT5 is a fructose-specific transporter in the glucose transporter family (GLUT, SLC2 gene family). Its substrate-specificity and tissue-specific expression make it a promising target for treatment of diabetes, metabolic syndrome and cancer, but few GLUT5 inhibitors are known. To identify and characterize potential GLUT5 ligands, we developed a whole-cell system based on a yeast strain deficient in fructose uptake, in which GLUT5 transport activity is associated with cell growth in fructose-based media or assayed by fructose uptake in whole cells. The former method is convenient for high-throughput screening of potential GLUT5 inhibitors and activators, while the latter enables detailed kinetic characterization of identified GLUT5 ligands. We show that functional expression of GLUT5 in yeast requires mutations at specific positions of the transporter sequence. The mutated proteins exhibit kinetic properties similar to the wild-type transporter and are inhibited by established GLUT5 inhibitors N-[4-(methylsulfonyl)-2-nitrophenyl]-1,3-benzodioxol-5-amine (MSNBA) and (−)-epicatechin-gallate (ECG). Thus, this system has the potential to greatly accelerate the discovery of compounds that modulate the fructose transport activity of GLUT5.
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ISSN:2045-2322
2045-2322
DOI:10.1038/s41598-017-06262-4