Chemical inhibitors of C12orf50 target various kinases involved in cell cycle regulation, thus impacting the activity of this protein. Alsterpaullone, Olomoucine, Roscovitine, Indirubin-3'-monoxime, Flavopiridol, Purvalanol A, CR8, and Dinaciclib share a common mechanism of action by inhibiting cyclin-dependent kinases (CDKs). These CDKs are integral to the regulation of the cell cycle, and their inhibition can disrupt the signaling pathways necessary for C12orf50 to function properly. Alsterpaullone, in particular, acts by targeting these kinases directly, therefore impeding the role of C12orf50 in cell cycle progression. Similarly, Olomoucine and Roscovitine serve to suppress CDK activity, leading to an indirect inhibition of C12orf50. This suppression can arrest the cell cycle, effectively limiting C12orf50's role in this vital process. Indirubin-3'-monoxime also blocks CDKs, which could be necessary for the regulatory function of C12orf50 in cell division, thereby inhibiting the protein by disrupting essential cell cycle signals.
Moreover, Flavopiridol and Purvalanol A inhibit CDKs, which are potentially crucial for C12orf50's activity in cell cycle control. By blocking these kinases, Flavopiridol can halt the cell cycle and indirectly inhibit the activity of C12orf50. Purvalanol A shares this inhibition pathway, obstructing cell cycle progression and signal transduction pathways where C12orf50 is involved. Beyond the realm of CDKs, TG003 targets CDC-like kinases (CLKs), which can influence the splicing of mRNA transcripts for various proteins, possibly including C12orf50. This inhibition can alter the processing of C12orf50's mRNA, thereby indirectly affecting its activity. Additionally, Harmine targets DYRK1A, which is involved in the phosphorylation of proteins within signaling pathways where C12orf50 may operate, thus indirectly inhibiting C12orf50. Lastly, 5-Iodotubercidin and AZD5438, through their action on adenosine kinases and CDKs respectively, can affect ATP-dependent processes and cell cycle progression, which are important for the functional activity of C12orf50, leading to its inhibition.
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