Date published: 2025-9-13

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G7c Activators

Chemical activators of G7c include a variety of compounds that promote its functional activation through different cellular signaling pathways and mechanisms. PMA, for instance, is a potent activator of Protein Kinase C (PKC), which in turn can phosphorylate G7c, leading to its activation. Similarly, Forskolin raises intracellular cAMP levels, which activate PKA, another kinase that can phosphorylate and thus activate G7c. The elevation of intracellular calcium levels by Ionomycin can activate calmodulin-dependent protein kinases, which may also target G7c for phosphorylation and activation. Inhibition of protein phosphatases by Okadaic Acid leads to increased phosphorylation levels within the cell, thereby maintaining G7c in an active state. Anisomycin, through its stimulation of stress-activated protein kinases, can likewise result in the phosphorylation and activation of G7c.

Further down the list, LY294002, by inhibiting PI3K, can lead to the activation of backup pathways that may phosphorylate and thus activate G7c. Rapamycin, an mTOR inhibitor, can have a similar effect, activating alternative kinases that can then target G7c. The plant hormone 6-Benzylaminopurine, known to activate cyclin-dependent kinases, could phosphorylate G7c as part of cell cycle regulation processes. Thapsigargin's role in disrupting calcium homeostasis can lead to kinase activation that targets G7c. Dibutyryl-cAMP, a stable cAMP analog, can activate PKA, which in turn can phosphorylate and activate G7c. Phosphatidic Acid, through its role in activating the mTOR signaling pathway, can also lead to the phosphorylation and activation of G7c. Lastly, Calyculin A, by inhibiting certain protein phosphatases, results in sustained phosphorylation of proteins including G7c, thus maintaining its active state. Each of these chemicals, through their unique interactions with various cellular components and pathways, can function as activators of G7c, facilitating its role in cellular processes.

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