Date published: 2025-9-11

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OR2T8 Inhibitors

Chemical inhibitors of Olfactory receptor 2T8 utilize a variety of mechanisms to impede the receptor's ability to detect and respond to odorant molecules. Naringenin and quercetin serve as direct antagonists to this receptor, with naringenin competitively binding to the odorant-binding site, thus preventing natural odorants from initiating a receptor response. Quercetin, on the other hand, employs an allosteric mechanism to alter the receptor's conformation, which decreases its sensitivity to activating molecules. This alteration in receptor conformation underscores the significance of the receptor's shape in its ability to function, as even slight modifications can inhibit its activity. Similarly, caffeine and resveratrol target the receptor indirectly; caffeine does so by modulating adenosine receptor activity, which in turn affects the intracellular signaling pathways essential for Olfactory receptor 2T8 activation. Resveratrol impacts the receptor's function by disrupting lipid raft composition, highlighting the critical role of the membrane's structural components in receptor localization and function. Moreover, compounds like curcumin, capsaicin, and menthol modify the receptor's microenvironment or its membrane fluidity, affecting the receptor's ability to undergo conformational changes for activation. Curcumin alters the receptor's microenvironment, potentially affecting its structural integrity, while capsaicin desensitizes the receptor, leading to temporary functional loss. Additionally, Gluconic acid zinc (II) salt and Copper(II) Sulfate inhibit the receptor by directly interacting with it. Lidocaine and sodium azide showcase the importance of ion channel activity and cellular respiration in receptor signal transduction, with lidocaine affecting ion channel function and sodium azide disrupting cellular energy mechanisms. Ethanol's role in modifying the lipid bilayer environment around Olfactory receptor 2T8 illustrates how changes in membrane dynamics can directly impact receptor function.

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