1810009A15Rik Activators encompass a curated set of chemical compounds that indirectly elevate the functional activity of 1810009A15Rik via distinct signaling pathways. Forskolin, IBMX, Dibutyryl-cAMP, and Rolipram all function primarily through the elevation of intracellular cAMP, thereby activating PKA, which is known to phosphorylate various substrates including those associated with 1810009A15Rik, resulting in its activation. PMA and Ionomycin, through the activation of PKC and increase of intracellular calcium levels respectively, also contribute to the activation of 1810009A15Rik by facilitating the phosphorylation of proteins that are part of 1810009A15Rik's functional framework. The influence of Okadaic Acid and Calyculin A on protein phosphatases leads to a phosphorylation bias, which could result in a more activated state of 1810009A15Rik due to decreased dephosphorylation rates.
Glucocorticoid Receptor Activators are a series of compounds that bind to and activate the receptor to induce a regulatory effect on gene transcription. Endogenous activator cortisol, alongside synthetic analogs such as prednisolone and dexamethasone, binds directly to the Glucocorticoid Receptor, causing conformational changes that facilitate its nuclear translocation and subsequent transcriptional activity on target genes. These compounds are structurally designed to mimic the natural ligand, providing a stronger and more prolonged activation of the receptor. Similarly, hydrocortisone and cortisone serve as endogenous activators, with cortisone being converted into the active form cortisol within the body, thereby promoting the receptor's activation. The synthetic glucocorticoids, betamethasone and triamcinolone, exhibit high receptor binding affinities, enhancing the Glucocorticoid Receptor-mediated gene expression related to anti-inflammatory processes and immunosuppression.
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