Forskolin and IBMX work by elevating cAMP levels, which can activate PKA and influence the phosphorylation state of numerous proteins, potentially altering the protein-protein interactions or post-translational modifications of REXO4. Similarly, growth factors like EGF can initiate signal transduction via EGFR, activating downstream pathways such as MAPK and PI3K, which could modify the activity or expression of proteins that associate with REXO4.
Phorbol esters like PMA, which mimic diacylglycerol, can activate PKC and subsequently alter the phosphorylation status of proteins that might interact with REXO4. Small molecule inhibitors such as SB203580, LY294002, SP600125, and U0126, which target MAPK, PI3K, JNK, and MEK1/2 respectively, demonstrate the interconnectedness of intracellular signaling pathways with RNA processing activities, as they may affect the regulation of REXO4 activity. Rapamycin, known for its role in mTOR inhibition, also impacts protein synthesis and RNA processing, potentially influencing REXO4's function in these processes. Epigenetic modifiers like 5-Azacytidine and Trichostatin A, as well as HDAC inhibitors such as Sodium Butyrate, can lead to changes in gene expression and chromatin dynamics that may alter the expression levels or the functional state of proteins that regulate or interact with REXO4.
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