Date published: 2025-9-13

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NPY2-R Activators

NPY2-R activators encompass a diverse class of chemicals that can influence the function or expression of this receptor indirectly through various mechanisms. These chemicals often target enzymes involved in the metabolism of secondary messenger molecules such as cAMP or guanosine 3',5'-cyclic monophosphate (cGMP), which play crucial roles in the signal transduction of G-protein coupled receptors (GPCRs) like NPY2-R. By elevating the levels of these secondary messengers, chemicals such as forskolin, IBMX, rolipram, and cilostamide can increase the signaling strength of NPY2-R. Similarly, chemicals that interact with the nitric oxide-cGMP pathway, such as YC-1, BAY 41-2272, ODQ, SNAP, L-NAME, and L-Arginine, can indirectly influence NPY2-R activity by modulating the function of soluble guanylyl cyclase, an enzyme that produces cGMP in response to nitric oxide. On the other hand, chemicals that affect the cellular response to hypoxia, such as echinomycin and KCN, can influence the expression of NPY2-R. By inhibiting HIF-1, echinomycin can prevent the upregulation of NPY2-R expression that occurs under hypoxic conditions. Conversely, KCN, by inducing a state of hypoxia, can promote HIF-1 activity and the subsequent upregulation of NPY2-R expression. These diverse mechanisms all contribute to thepotential activation of the NPY2-R receptor, offering numerous avenues for influencing its function. In summary, the category of NPY2-R activators is characterized by its diversity, with chemicals acting on different cellular processes to indirectly activate this receptor. Whether through the modulation of secondary messenger systems, or through the influence on cellular responses to hypoxia, these chemicals can interact with NPY2-R in an indirect manner. It's important to note, however, that the activation of NPY2-R by these chemicals is indirect and dependent on the context of cellular state and signaling pathways at play. This indirect activation provides a broader understanding of the complex regulatory networks that control NPY2-R activity and underscores the multifaceted nature of cellular signaling processes.

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