Date published: 2025-9-15

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MPc3_CBX8 Inhibitors

Chemical inhibitors of MPc3 can exert their inhibitory effects through the disruption of cell cycle regulation, given that MPc3's function is closely associated with cell cycle control. Compounds such as PD 0332991, Ribociclib, and Abemaciclib are all classified as CDK4/6 inhibitors, which directly target enzymes critical for the phosphorylation of the retinoblastoma protein (Rb). This phosphorylation event is a prerequisite for cell cycle progression from the G1 to the S phase, an area where MPc3 is known to operate. By inhibiting CDK4/6, these chemicals effectively induce G1 phase arrest, thereby curtailing the cellular context in which MPc3 exerts its function, leading to its functional inhibition. Similarly, Olomoucine and Roscovitine specifically target a range of CDKs including CDK1, CDK2, and CDK5, further contributing to cell cycle arrest and hence the functional inhibition of MPc3 by impeding the progression of phases that MPc3 is reliant upon.

Alsterpaullone and Purvalanol A, which are potent inhibitors of CDK1 and CDK2, also contribute to the impediment of cell cycle progression, thereby indirectly inhibiting the activity of MPc3. On the other hand, Dinaciclib and Milciclib broaden the scope of inhibition to include other CDKs and kinases like TrkA, which affect not only the cell cycle but also transcription regulation. This broad-spectrum inhibition disrupts cellular processes that are essential for MPc3's activity. Flavopiridol, by inhibiting CDKs, particularly affects transcription regulation that is linked to cell cycle progression, further contributing to the functional inhibition of MPc3. SNS-032 and AZD5438 extend this inhibition to CDKs that are crucial for both cell cycle transitions and transcription machinery, thereby creating a cellular environment that is non-conducive for MPc3 activity, leading to its functional inhibition.

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