Date published: 2025-9-13

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SPEC2 Activators

SPEC2 activators engage in various biochemical mechanisms to enhance the functional activity of the protein. Intracellular signaling molecules such as cyclic AMP (cAMP) play a pivotal role in the activation of SPEC2. Elevating intracellular cAMP levels through different means, including direct stimulation of adenylyl cyclase or inhibition of phosphodiesterases, leads to the activation of protein kinase A. This kinase is then capable of phosphorylating SPEC2, thus increasing its functional activity. Similarly, other compounds indirectly enhance cAMP levels by acting as agonists at adrenergic receptors, which subsequently stimulate intracellular adenylyl cyclase activity, again leading to PKA-mediated phosphorylation and activation of SPEC2. Furthermore, the inhibition of protein phosphatases that typically dephosphorylate proteins extends the phosphorylated state of SPEC2, indirectly contributing to its sustained activation.

Additional pathways that indirectly influence SPEC2 activity involve modulation of intracellular calcium levels and stress response mechanisms. Certain activators work by increasing intracellular calcium, which triggers calcium-dependent protein kinases that may target SPEC2 for phosphorylation. This calcium-mediated pathway is often initiated by compounds that stimulate calcium ionophores or activate ion channels that permit calcium influx into the cell. On another front, the inhibition of protein synthesis or the activation of stress-activated protein kinases through specific inhibitors and activators also leads to the activation of SPEC2. These stress response pathways can result in the phosphorylation of SPEC2, thereby altering its activity state.

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