Date published: 2025-9-15

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HEATR7B2 Activators

Activators of HEATR7B2 function by modulating intracellular signaling pathways, particularly those involving cyclic adenosine monophosphate (cAMP). Certain small molecules directly increase adenylyl cyclase activity, elevating cAMP levels and enhancing the activity of HEATR7B2 through cAMP-dependent pathways. Other compounds act as selective inhibitors of phosphodiesterases, which degrade cAMP, thus increasing its concentration and indirectly upregulating HEATR7B2 activity. Some of these molecules are selective for specific phosphodiesterase isoforms, while others have broader activity, impacting multiple isoforms to varying degrees. By preventing the breakdown of cAMP, these inhibitors facilitate sustained signaling through protein kinase A (PKA) and other cAMP-responsive elements, which are known to play a role in the pathways that HEATR7B2 is involved in.

Additionally, there are activators that function by engaging G protein-coupled receptors (GPCRs), leading to the production of cAMP via G protein signaling. For instance, agonists of adrenergic receptors can trigger this pathway, thereby promoting the activation of HEATR7B2. Certain eicosanoids also bind to their cognate GPCRs to elevate cAMP, further influencing the activity of HEATR7B2 through PKA-dependent mechanisms. Moreover, some activators are capable of directly mimicking the action of cAMP, bypassing upstream receptors and G proteins, and directly initiating signaling cascades that are likely to enhance the function of HEATR7B2.

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