Date published: 2025-9-14

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RPL39 Activators

Chemical activators of RPL39 engage in a series of interactions that result in the functional upregulation of this ribosomal protein's activity. Phorbol 12-myristate 13-acetate, for instance, activates protein kinase C (PKC), which is known to phosphorylate a variety of substrates, including ribosomal proteins, thereby enhancing their functionality in protein synthesis. Forskolin operates by elevating intracellular cAMP levels, which in turn activates PKA, another kinase that can phosphorylate RPL39, leading to an increase in its ribosomal activity. Similarly, ionomycin acts by increasing intracellular calcium concentrations, which triggers the activation of a cascade of calcium-dependent kinases. These kinases can also target RPL39, phosphorylating and activating it within the complex molecular machinery of the ribosome.

The role of protein phosphatases in the regulation of RPL39 cannot be understated, and several chemicals act by inhibiting these phosphatases, thereby ensuring RPL39 remains in a phosphorylated and active state. Okadaic Acid and Calyculin A both inhibit protein phosphatases such as PP1 and PP2A, which would otherwise dephosphorylate RPL39, leading to a decrease in its activity. Endothall and Cantharidin share a similar mechanism of action, inhibiting phosphatases and sustaining RPL39 in its active, phosphorylated form. Anisomycin activates stress-activated protein kinases which, upon activation, are known to phosphorylate various substrates, including those involved in ribosomal functions, like RPL39. Thapsigargin disrupts the calcium balance within the cell, leading to kinase activation that can result in the phosphorylation and consequent activation of RPL39. Lastly, Bisindolylmaleimide I and 4β-Phorbol, while primarily known for their interactions with PKC, can also ensure the activation of RPL39 through the kinase's phosphorylation activity. Mevalonolactone, through its role in the mevalonate pathway, can lead to biochemical modifications of proteins that interact with the ribosome, potentially resulting in the activation of RPL39 as these proteins carry out their roles in protein synthesis.

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