Date published: 2025-9-16

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SLC4A1AP Activators

Chemical activators of SLC4A1AP include a variety of compounds that can initiate a cascade of intracellular events leading to the activation of the protein. Forskolin is known to directly target adenylate cyclase, increasing the levels of cAMP within the cell. This rise in cAMP activates protein kinase A (PKA), a kinase that can phosphorylate SLC4A1AP, thereby enhancing its activity. Similarly, IBMX functions by inhibiting phosphodiesterases, enzymes responsible for cAMP breakdown, thus indirectly raising cAMP levels which subsequently activate PKA. PKA then targets SLC4A1AP for phosphorylation, leading to activation of its function. Dibutyryl-cAMP, a synthetic analog of cAMP, bypasses cell surface receptors and directly activates PKA, leading to subsequent phosphorylation and activation of SLC4A1AP.

In parallel, PMA, recognized as a potent activator of protein kinase C (PKC), can also lead to the phosphorylation and activation of SLC4A1AP. Activation of PKC through PMA triggers a series of phosphorylation events that can converge on SLC4A1AP. A23187, a calcium ionophore, elevates intracellular calcium levels, which in turn can activate calcium-dependent kinases capable of phosphorylating SLC4A1AP. Ionomycin acts in a similar manner to A23187, causing an increase in intracellular calcium and subsequent activation of kinases that can phosphorylate SLC4A1AP. Isoproterenol, through its agonistic action on beta-adrenergic receptors, also raises intracellular cAMP levels, further engaging PKA in the phosphorylation of SLC4A1AP. Calyculin A and Okadaic acid, both inhibitors of protein phosphatases, lead to a sustained phosphorylated state of proteins like SLC4A1AP by preventing their dephosphorylation, thus maintaining SLC4A1AP in an active form. Lastly, Genistein and LY294002 interfere with tyrosine kinase and PI3K signaling pathways, respectively, leading to changes in phosphorylation patterns that can result in the activation of SLC4A1AP through indirect but specific downstream effects. These chemicals provide a multi-faceted approach to the activation of SLC4A1AP through various signaling pathways and phosphorylation events.

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