Date published: 2025-9-15

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C6orf125 Activators

Chemical activators of C6orf125 can engage various cellular signaling pathways to initiate its activation. Forskolin, by escalating the levels of cAMP within the cell, directly stimulates adenylate cyclase, which in turn can enhance the activity of PKA. The activated PKA can then phosphorylate a range of substrates, including putatively C6orf125, thereby leading to its functional activation. Similarly, 8-Bromo-cAMP, as a cAMP analog, can also activate PKA, which further supports the phosphorylation and subsequent activation of C6orf125. In the realm of calcium signaling, Ionomycin, by serving as a calcium ionophore, raises intracellular calcium concentrations and can activate calcium-dependent kinases, which may target C6orf125 for phosphorylation. Thapsigargin, another modulator of calcium signaling, disrupts calcium homeostasis by inhibiting the SERCA pump, which leads to an increase in cytosolic calcium and could activate C6orf125 via downstream calcium-sensitive proteins.

The activation of protein kinase C (PKC) is another route through which C6orf125 can be activated. Phorbol 12-myristate 13-acetate (PMA) directly stimulates PKC, which could phosphorylate C6orf125. Bisindolylmaleimide I, even as a PKC inhibitor, can, under certain conditions, activate PKC, which may also lead to the phosphorylation and activation of C6orf125. The inhibition of protein phosphatases, such as PP1 and PP2A, by Calyculin A and Okadaic Acid, respectively, results in increased phosphorylation levels in the cell, potentially including the phosphorylation and activation of C6orf125. Anisomycin activates stress-activated protein kinases, like JNK, which can also target and activate C6orf125. Spermine, through its role in modulating ion channels and kinases, may facilitate the activation of C6orf125. Moreover, Zaprinast and Spermine NONOate, by increasing cGMP levels through the inhibition of PDE5 or the release of nitric oxide, respectively, can activate PKG, which in turn could phosphorylate and activate C6orf125, integrating nitric oxide and cGMP-dependent signaling pathways into the regulation of C6orf125 activity.

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