Date published: 2025-9-18

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ABHD1 Activators

Forskolin which by raising the levels of cAMP within the cell, sets off a chain reaction that can culminate in the activation of protein kinases such as PKA; these kinases are known to phosphorylate a range of targets and could potentially modify the activity of ABHD1 if it is within their substrate spectrum. PMA, specifically acts to stimulate protein kinase C (PKC), an enzyme capable of modifying numerous proteins through phosphorylation, and thus could influence ABHD1's activity by this modification if ABHD1 is indeed a PKC substrate. The action of ionomycin is another example, a compound that increases intracellular calcium, thus triggering the activation of a plethora of calcium-dependent kinases and potentially impacting the regulation of ABHD1 if it is sensitive to such calcium-mediated signaling. Meanwhile, isoproterenol and dibutyryl cAMP operate through mechanisms that increase cAMP, either via receptor-mediated pathways or by directly serving as a cAMP analog, respectively, thereby potentially affecting ABHD1's activity through cAMP-dependent pathways.

Additionally, the role of Sodium Orthovanadate as a phosphatase inhibitor suggests a potential for increased phosphorylation levels of proteins including ABHD1, assuming it has relevant tyrosine phosphorylation sites. LY294002, which impedes the PI3K pathway, could also influence ABHD1's activity if it is downstream of this particular signaling route. Furthermore, molecules like AICAR and 1,1-Dimethylbiguanide, Hydrochloride activate AMPK, which could alter ABHD1's function if AMPK signaling impacts ABHD1. Finally, polyphenolic compounds such as resveratrol, curcumin, and EGCG interact with cellular signaling through various mechanisms that include SIRT1 activation and histone deacetylase inhibition, suggesting that they could modify ABHD1 activity if it is regulated by such acetylation-related processes.

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