Date published: 2026-1-16

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EDA Activators

EDA Activators encompass a range of chemical compounds that indirectly augment the functional activity of EDA through various intracellular signaling pathways. Forskolin, cAMP, and IBMX all function to increase intracellular cAMP concentrations, a pivotal secondary messenger that activates protein kinase A (PKA). When activated, PKA can phosphorylate target proteins within the signaling pathways that EDA is associated with, thereby enhancing the overall activity of EDA by promoting the phosphorylation and subsequent activation of proteins downstream or upstream of EDA. Additionally, PMA and Ionomycin elevate the activity of protein kinase C (PKC) and intracellular calcium levels, respectively, which could modify the signaling cascades that indirectly modulate EDA's function by shifting the phosphorylation equilibrium of relevant proteins, thus influencing EDA activity.

The activity of EDA is further influenced by compounds that can alter the cellular phosphorylation landscape. Dibutyryl-cAMP, Rolipram, and Anisomycin lead to the accumulation of cAMP or activate stress-activated protein kinases that may indirectly influence EDA signaling. Okadaic Acid, by inhibiting phosphatases, and KN-93, by targeting CaMKII, can potentially lead to an enhanced phosphorylation state of proteins that interact with the EDA signaling pathway, potentially leading to increased EDA activity. BAPTA's role in modulating calcium levels could also impact the calcium-dependent kinases and phosphatases that are implicated in the pathways governing EDA's function, further potentiating the activation of EDA through these intricate signaling networks. Collectively, these chemical activators, through their targeted effects on key intracellular signaling components, facilitate the enhancement of EDA's functional activity without directly upregulating its expression or altering its primary structure.

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