Date published: 2025-9-21

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PPM1H Activators

PPM1H Activators are a select group of compounds that indirectly promote the functional activity of PPM1H, a serine/threonine phosphatase, by influencing the cellular phosphoprotein landscape. The accumulation of phosphorylated proteins, due to the action of Okadaic Acid and Calyculin A as inhibitors of PP1 and PP2A, creates an increased demand for PPM1H phosphatase activity. Similarly, compounds like Forskolin, Ionomycin, and Phorbol 12-myristate 13-acetate (PMA) activate signaling pathways that enhance protein phosphorylation, indirectly necessitating the dephosphorylation role of PPM1H. Forskolin, by increasing cAMP, and PMA, as a PKC activator, both contribute to an environment rich in phosphorylated proteins, which PPM1H then counteracts to maintain cellular function. Ionomycin's elevation of calcium levels can activate a plethora of kinases, thus indirectly enhancing PPM1H activity due to the resulting rise in phosphorylated proteins requiring dephosphorylation for cellular signaling reset.

Further on, the inhibition of protein phosphatases by Cantharidin, Endothall, and Tautomycin leads to a similar indirect upregulation of PPM1H activity as the cell compensates for the inhibited dephosphorylation pathway. Zoledronic Acid disrupts protein prenylation, potentially impacting signaling processes where PPM1H-mediated dephosphorylation is necessary. Anisomycin, through the activation of stress kinases, and Caffeine, by elevating cAMP levels, both contribute to a phosphorylation cascade that could amplify the demand for PPM1H's regulatory role. Lastly, Bisindolylmaleimide I, by inhibiting PKC, might create a unique phosphorylation pattern that requires PPM1H's activity to restore protein phosphorylation homeostasis. Collectively, these chemicals form a network of indirect activators that enhance PPM1H's role in cellular signaling by manipulating the balance of phosphorylation and dephosphorylation within the cell.

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