Date published: 2025-9-10

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Glut5 Inhibitors

Glut5 inhibitors include compounds that exert their influence through a variety of mechanisms to impede the activity of Glut5, a transporter protein primarily responsible for the uptake of fructose into cells. These inhibitors can work directly by binding to the transporter and blocking its fructose transport capacity, or indirectly by affecting the cellular signaling pathways that regulate the expression and trafficking of Glut5. Direct inhibition is characterized by a competitive or non-competitive blockade of the fructose binding site, which physically obstructs fructose from entering the cell via Glut5.

Indirect inhibitors, meanwhile, act through secondary mechanisms that ultimately downregulate or impair the function of Glut5. For instance, some inhibitors may impact the energy metabolism within the cell, altering the need and availability of fructose transport. Others may influence the insulin signaling pathway, which is known to regulate the abundance and activity of various glucose transporters, extending to Glut5. Additionally, certain compounds may inhibit kinases or other proteins involved in the post-translational modification of Glut5, thereby affecting its trafficking to the plasma membrane where it carries out its function. These inhibitors are not exclusively selective for Glut5 and may affect other transporters or cellular processes due to the interconnected nature of metabolic pathways. Their effectiveness can vary widely, depending on the cellular context, such as the type of cell, the presence of other sugars, and the overall metabolic state. Nonetheless, these compounds provide valuable tools for modulating fructose transport and studying the role of Glut5 in cellular metabolism.

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