Date published: 2025-9-10

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PAR-6 Activators

PAR-6 Activators are a diverse set of chemical compounds that indirectly enhance the activity of PAR-6, a pivotal protein in the regulation of cell polarity. Among these, Phorbol 12-myristate 13-acetate (PMA) serves as a potent PKC activator, which subsequently phosphorylates and activates PAR-6, bolstering its role in the formation of polarity complexes. Similarly, Forskolin, by escalating intracellular cAMP levels, activates PKA which may phosphorylate proteins that interact with PAR-6, thereby facilitating PAR-6's engagement in cell polarity. The GSK-3β inhibitor, 1-Azakenpaullone, may enhance PAR-6 signaling by preventing the phosphorylation of PAR-6's negative regulators. Y-27632, a ROCK inhibitor, and LY294002, a PI3K inhibitor, both function to dampen competing pathways, thereby indirectly potentiating PAR-6's involvement in cell adhesion and polarity. NSC 23766 curtails Rac1 activation, potentially stabilizing the PAR-6 complex, crucial for cell polarity maintenance. Sphingosine-1-phosphate and Thapsigargin, through lipid signaling and calcium mobilization, respectively, enhance the pathways that necessitate PAR-6's role in cell morphology and cytoskeletal organization.

Furthermore, the MEK inhibitor U0126 may indirectly facilitate PAR-6 function by altering the balance of intracellular signaling in favor of pathways that activate PAR-6. Go 6983, while generally inhibiting PKC, may preferentially support PAR-6 activity by selectively targeting specific PKC isoforms that negatively regulate cell polarity. Staurosporine, known for its broad kinase inhibition, can, at precise dosages, selectively inhibit kinases that otherwise suppress PAR-6 function, thereby indirectly promoting PAR-6's role in polarity. Finally, Bisindolylmaleimide I, by inhibiting negative regulatory PKC isoforms, may result in an upsurge in PAR-6 activity, underscoring the complexity and specificity of how these activators can converge on the pivotal cell polarity regulator PAR-6. Collectively, these compounds provide a framework for understanding the diverse mechanisms that can be leveraged to enhance PAR-6 activity without necessarily increasing its expression or direct activation.

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