Date published: 2025-9-14

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CDKN2AIP Activators

CDKN2AIP activators pivot around modulating the cell cycle, cellular senescence, and DNA damage response. Agents such as Forskolin, by influencing cAMP levels, and CDK inhibitors like Olomoucine and Roscovitine provide a framework for potential CDKN2AIP modulation by influencing cell cycle progression. DNA damage inducers, such as Etoposide and Cisplatin, underscore the tight link between DNA integrity and the regulation of proteins like CDKN2AIP, which can come into play upon DNA insult.

Lovastatin, while primarily known for its cholesterol-lowering ability, delves into cell cycle regulation by inhibiting HMG-CoA reductase, and thus may indirectly modulate CDKN2AIP. Similarly, Genistein, a phytoestrogen, traverses a myriad of cellular pathways, including cell cycle regulation, which can put CDKN2AIP in its purview. Microtubule modulators, Nocodazole, which disrupts, and Paclitaxel, which stabilizes, bring forth the importance of cytoskeletal integrity in maintaining cell cycle progression and the potential involvement of CDKN2AIP therein. Sulforaphane, another compound that induces cell cycle arrest, reinforces the prominence of CDKN2AIP in the intricate cell cycle landscape, emphasizing its indirect activation upon the modulation of various cell cycle checkpoints and related pathways.

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