Date published: 2025-9-14

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Gm1078 Activators

Uncharacterized serine/threonine-protein kinase SBK3 activators are a class of compounds that interact with a variety of cellular signaling pathways to potentially enhance the activity of SBK3. The mechanisms by which these activators work involve either direct enhancement of signaling pathways that lead to SBK3 activation or indirect effects through modulation of related pathways that result in an environment conducive to SBK3 activation. For instance, forskolin directly targets adenylyl cyclase to increase cAMP, which subsequently enhances PKA activity. PKA, being a kinase that phosphorylates a range of substrates, could phosphorylate SBK3 leading to its activation. IBMX complements this effect by inhibiting phosphodiesterase, thereby sustaining increased levels of cAMP and enhancing PKA-mediated activation of SBK3.

The inhibitors of GSK-3, such as Lithium Chloride and SB 216763, may indirectly enhance SBK3 activity by affecting the balance of kinase and phosphatase activities within the cell, which can lead to the activation of SBK3. Inhibitors of epigenetic modifiers like 5-Azacytidine and Trichostatin A can lead to the upregulation of kinases, potentially including SBK3, by changing the transcriptional landscape in favor of its activation. Furthermore, compounds like LY294002, U0126, and PD 98059 that inhibit various kinases such as PI3K, MEK, and mTOR respectively, can disrupt established feedback loops and signaling cascades, potentially creating a cellular state that favors SBK3 activation. Additionally, BIX 02189's inhibition of MEK5 could impact ERK5 signaling, leading to a rebalanced kinase activity that enhances SBK3 activity.

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