Date published: 2025-9-15

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TRPC7 Inhibitors

TRPC7 inhibitors encompass a range of chemicals that indirectly modulate the function and activity of TRPC7, a transient receptor potential cation channel involved in various cellular signaling processes. These inhibitors typically function by altering the ionic homeostasis and membrane potential dynamics that are central to TRPC7's activity. For example, SKF-96365 and Ruthenium Red, both non-selective TRP channel blockers, inhibit calcium influx through TRPC7, thereby modulating its activity. Similarly, compounds like 2-APB, La3+, and Gadolinium influence TRPC7 by modulating ion permeability and calcium homeostasis, impacting the channel's function in cellular signaling. Other inhibitors, such as Econazole and Flufenamic Acid, which are known to block TRP channels, can reduce TRPC7-mediated calcium influx, affecting its role in cellular processes. Calcium channel blockers like Mibefradil, Nifedipine, and Verapamil, though primarily targeting other calcium channels, can indirectly influence TRPC7 activity by modulating overall calcium signaling within cells. Additionally, Capsazepine, a TRPV1 antagonist, and Menthol, a known modulator of TRP channels, represent another approach to modulating TRPC7 activity by affecting the dynamics of the TRP channel family.

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