Date published: 2025-11-1

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Vmn2r68 Activators

Chemical activators of Vmn2r68 can engage in various pathways to elicit an activation response in the protein. Cyclic AMP, for example, is a key secondary messenger involved in the activation of protein kinase A (PKA). PKA is known to phosphorylate numerous proteins, and through this mechanism, it can activate Vmn2r68. Similarly, Forskolin directly targets adenylate cyclase, enhancing the production of cAMP, and thus fosters a conducive environment for the activation of PKA, which subsequently can activate Vmn2r68. Isoproterenol and Epinephrine both work through adrenergic receptors to escalate cAMP levels, thereby promoting PKA activity, which can result in the activation of Vmn2r68. Histamine, when it interacts with its H2 receptors, and Dopamine, through its D1-like receptors, both increase cAMP production. This elevation in cAMP facilitates the activation of PKA, creating the necessary conditions for the activation of Vmn2r68.

Furthermore, Adenosine, by interacting with A2A receptors, can also raise cAMP levels and sustain PKA activity, leading to the activation of Vmn2r68. IBMX and Rolipram both inhibit phosphodiesterases, the enzymes responsible for degrading cAMP, thereby maintaining an activated state of PKA, which can then activate Vmn2r68. Glucagon, through its receptor, and Prostaglandin E2, by engaging with EP2 and EP4 receptors, are additional examples of chemicals that increase cAMP and activate PKA, which in turn can activate Vmn2r68. Lastly, Terbutaline, as a Beta2-adrenergic agonist, increases cAMP production, ensuring that PKA remains active to facilitate the activation of Vmn2r68. Each of these chemicals contributes to the regulation and activation of Vmn2r68 through the modulation of cAMP levels and the subsequent activation of PKA, demonstrating the intricate network of intracellular signaling pathways that can converge on the activation of this specific protein.

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