Date published: 2025-9-15

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Vmn2r118 Activators

Chemical activators of Vmn2r118 can engage various signalling pathways to elicit their effects. Forskolin is a potent activator of adenylyl cyclase, thereby increasing the intracellular levels of cyclic AMP (cAMP), a second messenger that is pivotal in the activation of protein kinase A (PKA). PKA can phosphorylate target proteins, including Vmn2r118, leading to its functional activation. Similarly, Isoproterenol, a beta-adrenergic agonist, enhances cAMP production through the stimulation of adenylyl cyclase which activates PKA. Upon activation, PKA can phosphorylate Vmn2r118 directly, resulting in its activation. Epinephrine, which binds to adrenergic receptors, also induces adenylyl cyclase activity, raising cAMP concentrations. The ensuing PKA activation then phosphorylates Vmn2r118, triggering its activation. Histamine, through its action on H2 receptors, stimulates Gs proteins that are coupled to adenylyl cyclase, leading to increased cAMP and subsequent PKA-mediated activation of Vmn2r118.

Dopamine interacts with D1-like receptors that activate adenylyl cyclase through Gs proteins, leading to PKA activation which then phosphorylates and activates Vmn2r118. Glucagon similarly exerts its effects by binding to its specific receptor, subsequently engaging Gs proteins that activate adenylyl cyclase, raising cAMP levels, and activating PKA, which in turn phosphorylates and activates Vmn2r118. Inhibitors of phosphodiesterases like IBMX, Rolipram, Cilostamide, and Anagrelide result in elevated cAMP levels by preventing the breakdown of cAMP to its inactive form. The resulting sustained activity of PKA can phosphorylate Vmn2r118, leading to its activation. Prostaglandin E1 (Alprostadil) activates adenylyl cyclase via E-prostanoid receptors and Gs proteins, which increases cAMP and activates PKA, subsequently leading to the phosphorylation and activation of Vmn2r118. Lastly, Vinpocetine, by inhibiting phosphodiesterase-1, causes an increase in cAMP, which activates PKA, and this kinase then activates Vmn2r118 through phosphorylation. Each of these chemicals, through their unique interactions with cellular signaling pathways, ultimately promotes the activation of Vmn2r118 in a specific manner.

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