Date published: 2025-9-14

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OPAL1 Activators

OPAL1 Activators encompass a diverse array of chemical compounds that serve to enhance the activity of OPAL1 through various biochemical mechanisms. For example, cyclic AMP (cAMP), a well-known second messenger, can activate protein kinase A (PKA), which is capable of phosphorylating numerous proteins, thereby potentially increasing the functional activity of OPAL1. Similarly, Phorbol 12-myristate 13-acetate (PMA) is an activator of protein kinase C (PKC), which can initiate a cascade of phosphorylation events that may lead to the activation of OPAL1. Forskolin, by stimulating adenylyl cyclase, raises intracellular cAMP levels, leading to PKA activation and subsequent enhancement of OPAL1 activity. Ionomycin, through the elevation of intracellular calcium levels, may activate calcium-dependent protein kinases that could in turn enhance OPAL1 activity. Retinoic acid, by modulating gene expression through its receptors, may cause post-translational modifications that activate OPAL1, while Zinc pyrithione could potentially activate OPAL1 through its role in zinc signaling.

Further, compoundslike Spermidine, which influences autophagy, could indirectly lead to the activation of OPAL1 by modulating cellular degradation and renewal processes. Epigallocatechin gallate (EGCG), a known kinase inhibitor, may enable the activation of OPAL1 by preventing inhibitory phosphorylations or by releasing OPAL1 from inhibitory protein-protein interactions that suppress its activity. Curcumin is another agent that can intersect with various signaling pathways, such as those involved in managing cellular stress responses, potentially resulting in the enhancement of OPAL1 activity by stabilizing the protein or activating related pathways. Nicotinamide adenine dinucleotide (NAD+), as a pivotal coenzyme in redox reactions, might indirectly influence OPAL1 activity by altering the metabolic state of the cell and consequently affecting protein functions. Hydrogen peroxide (H2O2), in low concentrations, acts as a signaling molecule that can enhance OPAL1 activity through the modulation of redox-sensitive signaling pathways or by activating oxidative stress response mechanisms. Lastly, nitric oxide donors like SNAP contribute to the activation of OPAL1 through processes such as S-nitrosylation or by modulating signaling pathways that regulate protein activity, highlighting the multifaceted nature of OPAL1 activators and their potential to influence OPAL1 through different biochemical routes.

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