Date published: 2025-9-16

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TMEM151B Inhibitors

Chemical inhibitors of TMEM151B include a variety of compounds that inhibit the protein through different mechanisms related to the protein's function and interaction with the cellular membrane. Phloretin disrupts glucose transport across the cell membrane, which can also affect the transport function of TMEM151B by altering the membrane's permeability or transporter conformation. Genistein acts as a tyrosine kinase inhibitor, preventing the phosphorylation that is often essential for the activation and function of membrane proteins, thus it can inhibit the activation state of TMEM151B. Quercetin, with its kinase inhibitory properties, can interfere with kinases that are responsible for phosphorylating TMEM151B or those within its regulatory pathways, leading to an inhibition of TMEM151B's activity.

Bisphenol A affects membrane integrity and fluidity, which can alter TMEM151B's conformation and function within the lipid bilayer. Chlorpromazine changes the lipid composition of membranes, potentially inhibiting TMEM151B's integration or function within the membrane. W-7 Hydrochloride, by inhibiting calmodulin, can disrupt the regulatory interactions essential for TMEM151B's function. Calcium channel blockers like Verapamil, Diltiazem, and Nifedipine can inhibit TMEM151B by affecting calcium-dependent regulatory mechanisms that could be crucial for TMEM151B's function. Propranolol disrupts lipid bilayer properties and interferes with signaling pathways that may be related to TMEM151B's function, while Amiloride directly interferes with ion transport mechanisms in membranes, which could be closely associated with TMEM151B's activity. Lastly, Omeprazole, as a proton pump inhibitor, alters the pH gradient across the membrane, which can influence the environment necessary for TMEM151B's proper function. Each of these chemicals targets specific aspects of membrane-associated processes and signaling that are crucial for the functional activity of TMEM151B, leading to its inhibition.

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