Date published: 2025-12-22

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ZC3H12D Activators

ZC3H12D Activators encompass a collection of chemical compounds that indirectly amplify the ribonuclease activity of ZC3H12D through various cellular signaling pathways. cAMP-elevating agents such as Forskolin, Rolipram, and IBMX, through their inhibition of phosphodiesterases, lead to an increase in PKA activity. This heightened PKA activity may facilitate the phosphorylation of proteins involved in RNA turnover, a process in which ZC3H12D plays a pivotal role. Similarly, AMPK activators like A-769662 and Metformin may indirectly enhance ZC3H12D's function in mRNA decay by affecting metabolic pathways that intersect with RNA regulation. GSK-3β inhibitors such as Lithium and SB 216763 have the potential to modify the mRNA stability landscape by influencing proteins that ZC3H12D interacts with, thereby enhancing its ability to regulate mRNA decay.

PMA, EGCG, Curcumin, Resveratrol, and Spermidine, exert their effects through diverse mechanisms, yet convergently enhance ZC3H12D function. PMA's activation of PKC may lead to the phosphorylation of substrates that impact RNA-binding proteins, thereby indirectly facilitating ZC3H12D's role in mRNA stability. Kinase inhibitors like EGCG, through theirbroad-spectrum action, could modify signaling pathways that affect proteins linked to ZC3H12D, potentially boosting its activity. Curcumin's modulation of various signaling pathways might also alter the interaction landscape of ZC3H12D, enhancing its regulatory capacity. Through SIRT1 activation, Resveratrol could lead to deacetylation of key proteins in RNA metabolism, indirectly enhancing ZC3H12D's function. Lastly, Spermidine's ability to induce autophagy could influence the activity of RNA-binding proteins that interact with ZC3H12D, thereby modulating its role in the mRNA decay process. Collectively, these ZC3H12D Activators exert their influence by targeting specific cellular processes that, in turn, enhance the functional activity of ZC3H12D in mRNA regulation.

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