Date published: 2025-9-20

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Olr1714 Activators

Chemical activators of Olr1714 can initiate a cascade of intracellular events leading to the protein's activation. Forskolin is one such activator that directly targets adenylyl cyclase to increase cAMP levels, subsequently activating protein kinase A (PKA). PKA is a key enzyme that phosphorylates Olr1714, thus activating it. Similarly, both Dibutyryl-cAMP and 8-Bromo-cAMP, as cAMP analogues, bypass upstream receptors and adenylyl cyclase to directly activate PKA, which in turn activates Olr1714 through phosphorylation. Another chemical, Ionomycin, facilitates an influx of calcium ions, which activates calcium/calmodulin-dependent protein kinases. These kinases then phosphorylate and activate Olr1714. Furthermore, Thapsigargin and BAY K8644 enhance intracellular calcium levels, either by inhibiting the SERCA pump or by activating L-type calcium channels, respectively, leading to the activation of Olr1714 through kinase-mediated phosphorylation.

Phorbol 12-myristate 13-acetate (PMA) activates protein kinase C (PKC), which is another kinase capable of phosphorylating Olr1714, leading to its activation. In a different approach, Okadaic Acid and Sodium Fluoride function by inhibiting protein phosphatases, preventing the dephosphorylation and thus maintaining Olr1714 in an active phosphorylated state. Anisomycin is another chemical that indirectly activates Olr1714 by activating stress-activated protein kinases such as JNK and p38 MAP kinases, which phosphorylate target proteins including Olr1714. Zinc Sulfate, by increasing intracellular zinc concentration, can activate multiple kinases that phosphorylate Olr1714, leading to its activation. Lastly, H-89 dihydrochloride, although primarily a PKA inhibitor, can lead to compensatory cellular responses that activate Olr1714 through alternative pathways. Each of these chemicals, through their specific actions on cellular enzymes and ions, play a distinct role in ensuring the phosphorylation and subsequent activation of Olr1714.

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