Date published: 2025-10-11

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XLαs Activators

XLαs Activators comprise a specialized group of chemical compounds that each contribute to the enhancement of XLαs signaling through various mechanisms. Forskolin, known for its direct activation of adenylyl cyclase, leads to an increase in cyclic AMP (cAMP) levels within cells. This cascade of events triggers the activation of protein kinase A (PKA), which is likely to enhance the signaling pathways that are regulated by XLαs, resulting in increased functional output of this protein. Another notable compound, 3-Isobutyl-1-methylxanthine (IBMX), operates by inhibiting phosphodiesterases, thereby preventing the degradation of cAMP and sustaining the signaling cascade that XLαs is a part of. This action ensures a prolonged and enhanced functional state of XLαs. Similarly, agonists like Isoproterenol and Epinephrine stimulate beta-adrenergic receptors, which are coupled with Gs proteins, leading to the activation of adenylyl cyclase and subsequent increase in cAMP. This process, in turn, amplifies the activity of XLαs by promoting the signaling pathways it influences.

Additional compounds such as Prostaglandin E2 (PGE2), Salbutamol, and Dopamine (at D1 receptors) also modulate Gs protein-coupled receptors, triggering adenylyl cyclase activation and fostering an environment that favors XLαs activity. The actions of Histamine at H2 receptors, Glucagon, Terbutaline, and Adenosine at A2 receptors further illustrate the diversity of mechanisms that lead to increased cAMP levels, which is a crucial factor in the functional enhancement of XLαs. Lastly, Rolipram, by selectively inhibiting phosphodiesterase-4, effectively raises cAMP levels, thereby contributing to the sustained activation of XLαs-mediated signaling pathways. Collectively, these XLαs Activators, through their targeted effects on the cAMP signaling cascade and related pathways, ensure the augmentation of XLαs function without the need to increase its expression or direct activation.

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