Date published: 2025-9-14

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RSAD1 Activators

Forskolin and Dibutyryl-cAMP serve as key players in elevating the levels of cAMP, a pivotal secondary messenger that orchestrates a range of signaling pathways that intertwine with RSAD1's regulation. By elevating cAMP, these compounds set the stage for cAMP-dependent protein kinases to activate and potentially engage with RSAD1 or its associated proteins. PMA, targets protein kinase C, which is instrumental in phosphorylating an array of proteins, thereby possibly altering the activity of RSAD1 if it lies within PKC's influential sphere. Ionomycin complements this by increasing intracellular calcium concentration, triggering calcium-dependent signaling pathways that could intersect with RSAD1's operational network. Insulin catalyzes a signaling domino effect that activates the PI3K/AKT pathway, a critical route that can dictate RSAD1's activation state by influencing its phosphorylation status. Similarly, EGF by engaging its receptor ignites a signaling cascade with potential repercussions for RSAD1's activity.

Lithium Chloride and SB 216763, GSK-3 inhibitors, are thought to contribute to the stabilization and consequent activation of RSAD1 by preventing its phosphorylation-dependent degradation. This preemptive action against degradation allows RSAD1 to maintain its functional state within the cell. Curcumin and Resveratrol are multifaceted in their approach, capable of altering the activity of RSAD1 through varied mechanisms, including the modulation of transcription factors or the acetylation of proteins that are part of RSAD1's signaling landscape. Sodium Salicylate, by inhibiting NF-κB, a regulator known to suppress certain proteins, may indirectly foster a more active state of RSAD1. 8-Bromo-cAMP ability to serve as a cAMP analogue, reinforcing the role of cAMP-dependent pathways in the potential activation of RSAD1.

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