Date published: 2025-9-15

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GLB1L3 Activators

GLB1L3 Activators are a set of chemical entities that indirectly promote the functional activity of GLB1L3 through specific signaling pathways. Compounds like Forskolin and Rolipram facilitate the elevation of cAMP, thus activating PKA, which can result in the phosphorylation and consequent activation of GLB1L3. IBMX compounds this effect by inhibiting the degradation of cAMP and cGMP, leading to a sustained activation of PKA and PKG pathways that could further enhance GLB1L3's activity. Epigallocatechin gallate and Sildenafil exert their influence by modulating acetylation states and cGMP levels, respectively, which could create an environment conducive to the upregulation of GLB1L3 activity. Sildenafil, in particular, by specifically increasing cGMP, may engage PKG signaling pathways that influence GLB1L3.

Additionally, the activities of GLB1L3 are potentially bolstered by chemicals that affect cellular dynamics and second messenger systems. Y-27632, through the inhibition of ROCK kinase, alters cytoskeletal arrangements, potentially enhancing the function of mechanosensitive entities like GLB1L3. A23187, by increasing intracellular calcium, could activate calcium-dependent proteins, including GLB1L3. PMA, by activating PKC, may phosphorylate proteins within the PKC signaling pathway, indirectly influencing GLB1L3 activity. In a nuanced interplay, LY294002 and Staurosporine modulate various kinase pathways, with potential upregulation of GLB1L3 function, while Ouabain shifts ion gradients, potentially triggering signaling cascades that lead to the activation of GLB1L3.

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