Date published: 2025-12-23

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V1RI7 Inhibitors

V1RI7 Inhibitors are a diverse group of chemical compounds that exert their effects by attenuating the signaling pathways and biological processes in which V1RI7 is involved. For example, Epigallocatechin gallate, with its phosphodiesterase-inhibiting properties, leads to elevated cAMP levels, which could subsequently downregulate V1RI7 activity due to altered intracellular signaling dynamics. Similarly, LY294002 acts as a PI3K inhibitor, thereby dampening the PI3K/Akt pathway, a crucial regulator of various cellular processes, including those linked to GPCR pathways where V1RI7 may participate. This attenuation could result in decreased V1RI7 signaling. U0126 and PD98059, both MEK inhibitors, potentially decrease V1RI7 activity by preventing the activation of ERK1/2, which could be part of V1RI7-mediated signaling events. SB203580, a p38 MAPK inhibitor, may suppress V1RI7 activity by affecting the cytokine milieu and inflammatory responses, which can modulate the receptor's function.

Additional inhibitors like Rapamycin and Y-27632 impact V1RI7 through different mechanisms. Rapamycin inhibits mTOR, leading to a reduction in the synthesis of proteins that form part of the V1RI7 signaling cascade, while Y-27632, as a ROCK inhibitor, could decrease V1RI7-related smooth muscle contractility. Clozapine's antagonistic action on dopamine receptors may indirectly influence V1RI7 activity by altering dopaminergic signaling. Chelerythrine and Go 6983, both targeting PKC, could reduce V1RI7 signaling by diminishing the phosphorylation states of proteins in the pathway. Lastly, BAPTA-AM, by chelating intracellular calcium, has the potential to inhibit V1RI7.

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