Date published: 2025-9-14

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TRIM12 Activators

Chemical activators of TRIM12 can exert their influence through a variety of cellular signaling pathways by either raising intracellular messenger levels or by modifying enzyme activity directly related to the phosphorylation state of the protein. Phorbol 12-myristate 13-acetate (PMA) and Prostratin are known to activate Protein Kinase C (PKC), which can phosphorylate TRIM12, leading to its functional activation. PKC serves as a pivotal kinase in the activation of numerous proteins through phosphorylation, thus playing a critical role in the regulation of TRIM12 activity. Similarly, Forskolin and 8-Bromo-cAMP, by increasing intracellular cAMP, activate Protein Kinase A (PKA), another kinase that can phosphorylate TRIM12. Activation of PKA is a well-established mechanism by which proteins can be phosphorylated and thus functionally activated.

Additionally, the modulation of intracellular calcium levels by chemicals such as Ionomycin, Thapsigargin, and A-23187 (Calcimycin) can also initiate a cascade of events leading to the activation of TRIM12. These chemicals increase cytosolic calcium, which in turn can activate calcium-responsive signaling molecules that phosphorylate TRIM12. Anisomycin, by activating the JNK/SAPK pathway, and U0126, by engaging the ERK/MAPK pathway, can similarly lead to the phosphorylation of TRIM12, albeit through different signaling routes. SB 203580, while primarily a p38 MAPK inhibitor, can induce compensatory mechanisms in cell signaling that may result in the activation of alternative kinases capable of activating TRIM12. Okadaic Acid, on the other hand, prevents dephosphorylation by inhibiting protein phosphatases, thus promoting the phosphorylated and active state of TRIM12. Lastly, Bisindolylmaleimide I (BIM I), although a PKC inhibitor, can induce activation of alternative pathways that can culminate in the activation of TRIM12, showcasing the intricate network of kinase and phosphatase activities that control protein activation states.

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