Date published: 2025-10-11

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Vmn2r37 Activators

Chemical activators of Vmn2r37 can be diverse in structure but share a common mechanism of action that leads to the activation of the protein. Forskolin, a diterpene, directly stimulates the activation of adenylyl cyclase, resulting in an increased production of cyclic AMP (cAMP). Elevated levels of cAMP lead to the activation of protein kinase A (PKA), which is known to phosphorylate and thereby activate Vmn2r37. Similarly, Isoproterenol, a synthetic catecholamine, binds to and activates beta-adrenergic receptors, which also stimulate adenylyl cyclase and increase cAMP levels, resulting in PKA-mediated activation of Vmn2r37. Histamine engages H2 receptors that follow the same cAMP-mediated pathway, resulting in PKA activation and subsequent phosphorylation of Vmn2r37. Additionally, Glucagon, a peptide hormone, binds to its receptor to increase cAMP and activate PKA, which in turn phosphorylates and activates Vmn2r37.

Inhibition of cAMP breakdown also plays a role in activating Vmn2r37. IBMX, a non-selective phosphodiesterase inhibitor, prevents cAMP degradation, which contributes to the sustained activation of PKA and the downstream activation of Vmn2r37. Rolipram and Cilostamide are more selective phosphodiesterase inhibitors targeting PDE4 and PDE3, respectively, and both establish increased cAMP levels that activate PKA, leading to Vmn2r37 activation. Vinpocetine, another selective PDE inhibitor, targets PDE1 to enhance cAMP levels, again activating PKA and promoting the activation of Vmn2r37. Epinephrine and Dopamine, both catecholamines, interact with their respective receptors to trigger adenylyl cyclase, raise cAMP levels, activate PKA, and facilitate the activation of Vmn2r37. Alprostadil, through its action on E-prostanoid receptors, increases cAMP and activates PKA, which can activate Vmn2r37. Finally, Anagrelide, by inhibiting PDE3 and increasing cAMP, leads to PKA activation, phosphorylating and activating Vmn2r37. Each of these chemicals facilitates a rise in cAMP levels, which is a crucial second messenger in the signaling pathway that leads to the activation of Vmn2r37.

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