Date published: 2025-9-10

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SLC-1 Inhibitors

Chemical inhibitors of the protein SLC-1 operate through various mechanisms to impede its function as a glucose transporter in yeast. Phloretin, a dihydrochalcone, can inhibit SLC-1 by interfering with the translocation of glucose across the cell membrane, while Cytochalasin B disrupts the actin cytoskeleton, essential for the proper localization and function of SLC-1 on the membrane. Quercetin and Apigenin, both of which are plant flavonoids, can bind to the glucose transporters and inhibit the uptake of glucose, thereby inhibiting the activity of SLC-1. Similarly, Genistein, an isoflavone, can affect the activity of glucose transporters, leading to the inhibition of SLC-1's role in glucose transport. Phlorizin, a glucoside, can competitively inhibit SLC-1 by binding to the glucose binding site on the transporter, effectively blocking glucose from entering the cell.

Other chemical inhibitors like WZB117 and BAY-876 specifically target glucose transporters, binding to them to prevent glucose from entering the cell, thereby inhibiting SLC-1 activity. Fasentin also interferes with the glucose transport mechanism and can prevent SLC-1 from transporting glucose into cells. STF-31, known for its inhibitory action on glucose transporters, can bind to SLC-1 and impede glucose uptake. Ritanserin, while primarily known as a serotonin receptor antagonist, can inhibit glucose transporters and thus can inhibit SLC-1 by obstructing glucose transport. Lastly, Indinavir, an HIV protease inhibitor known to interact with and inhibit GLUT4, a mammalian glucose transporter, can inhibit SLC-1 by a similar mechanism, possibly through altering the transporter's conformation or function, leading to reduced transport of glucose. These diverse chemicals can inhibit SLC-1, each utilizing a unique approach to disrupt the normal function of glucose transport into the cell.

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