Date published: 2025-9-15

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KCTD13 Activators

KCTD13 Activators in neuronal signaling and development are characterized by a diverse array of chemical compounds that indirectly stimulate the functional activity of KCTD13 through nuanced modulation of intracellular signaling pathways. Compounds such as Forskolin and Rolipram elevate and maintain cAMP levels, respectively, leading to the activation of PKA, which is hypothesized to enhance KCTD13 activity by phosphorylation mechanisms pivotal to neurodevelopment and synaptic plasticity. Dibutyryl-cAMP directly stimulates PKA, resulting in increased phosphorylation and subsequent activation of KCTD13. Epigallocatechin gallate, with its kinase inhibitory properties, and Ionomycin, through elevation of intracellular calcium levels, may indirectly augment KCTD13 activity by modifying the cellular signaling landscape, thereby favoring KCTD13's role in neuronal signaling. Moreover, Curcumin, by affecting PKC and other pathways, could potentiate KCTD13's function within the central nervous system, considering that PKC is integral to numerous neuronal processes.

In addition, Isoproterenol, as a beta-adrenergic receptor agonist, heightens cAMP in neuronal cells, thereby indirectly facilitating KCTD13-mediated regulation of synaptic vesicle dynamics. The action of PMA as a PKC activator could lead to phosphorylation of proteins within the pathways in which KCTD13 operates, promoting its synaptic efficacy. BAPTA-AM, by modulating intracellular calcium, can indirectly affect the function of KCTD13 in neurotransmission, while retinoic acid, by impacting gene expression during neuronal differentiation, may elevate KCTD13 activity linked to developmental pathways. Lastly, the MEK inhibitor PD 98059 and PI3K inhibitor LY294002 may indirectly amplify KCTD13's synaptic role by modulating the MEK/ERK and PI3K/Akt pathways, which are implicated in synaptic plasticity and formation, where KCTD13 is believed to be functionally significant. Together, these activators constitute a chemically varied group that, through their targeted effects on signaling pathways, facilitate the upregulation of KCTD13's activity without necessitating direct binding or upregulation of expression.

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