Date published: 2025-9-12

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WDR22 Activators

WDR22 (DDB1 and CUL4 associated factor 5) activators engage with diverse cellular signaling pathways to enhance its functional activity. Compounds that elevate intracellular cAMP levels do so by activating adenylate cyclase or inhibiting phosphodiesterase, leading to an environment conducive to the stabilization of WDR22 through cAMP-dependent mechanisms. cAMP analogs further reinforce this effect by mimicking the action of cAMP and activating protein kinase A (PKA), which may then phosphorylate downstream proteins that directly or indirectly stabilize WDR22. Additionally, activators that target protein kinase C (PKC) could phosphorylate a range of substrate proteins, potentially including those that interact with WDR22, thereby increasing its activity. The interaction of WDR22 with 14-3-3 proteins, a family known for their role in stabilizing various client proteins, may be enhanced by compounds that stabilize this interaction, thereby potentially increasing the functional activity of WDR22.

Further, activators that modulate intracellular calcium levels, either by acting as ionophores or by stabilizing calcium-binding proteins, might influence the activity of WDR22 through calcium-dependent signaling pathways. Inhibition of GSK-3 by certain compounds could lead to the stabilization of a suite of proteins, potentially including WDR22, while inhibitors of protein phosphatases such as PP1 and PP2A might increase the phosphorylation state of proteins that are involved in WDR22 activation. In response to cellular stress signals, activators that stimulate stress-activated protein kinases could also induce phosphorylation events that regulate proteins associated with WDR22, thereby modulating its activity. Furthermore, the use of MEK inhibitors could result in an increase in ERK activity which might influence the phosphorylation and activation of WDR22, while other compounds might induce compensatory mechanisms within the cell that ultimately lead to the stabilization and increased activity of WDR22.

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