Date published: 2025-9-11

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C2orf30 Inhibitors

Chemical inhibitors of C2orf30 target various aspects of cell cycle regulation, a process in which this protein is involved. Palbociclib, a selective inhibitor of cyclin-dependent kinases CDK4 and CDK6, disrupts the cell cycle progression, leading to the inhibition of C2orf30 function. This is because C2orf30's activity is closely tied to the cell cycle, and by halting the cycle, Palbociclib effectively hinders the protein's role. Similarly, Roscovitine targets a broad spectrum of CDKs, which are essential for controlling the progression of the cell cycle. By inhibiting these kinases, Roscovitine can suppress the function of C2orf30. Alsterpaullone also acts as a potent inhibitor of CDKs, and in doing so, can inhibit the function of C2orf30 by impeding the cell cycle processes that this protein facilitates.

Continuing along the same mechanism, Indirubin, Olomoucine, and Flavopiridol serve as inhibitors of CDKs. The inhibition of these kinases by Indirubin and Olomoucine can inhibit the function of C2orf30 by preventing the cell cycle events that C2orf30 is associated with. Flavopiridol, with its ability to inhibit several CDKs, disrupts cell cycle regulation and in turn, the function of C2orf30. Ribociclib and PD0332991 (Palbociclib) specifically inhibit CDK4/6 and by interfering with these particular kinases, they can inhibit the function of C2orf30 through the disruption of cell cycle events. AT7519, a multi-CDK inhibitor, can inhibit the function of C2orf30 by interfering with the general progression of the cell cycle. Milciclib, which affects various CDKs, can prevent the cell cycle-related functions of C2orf30, thus inhibiting the protein's function. Furthermore, Dinaciclib, a potent inhibitor of several CDKs, affects cell cycle control, leading to the inhibition of C2orf30. Lastly, SNS-032, by selectively inhibiting CDKs 2, 7, and 9, disrupts processes central to C2orf30's role in cell cycle regulation, achieving the inhibition of the protein's function. Each of these chemicals exerts its inhibitory effect by targeting the cell cycle, subsequently hindering the functional role of C2orf30 within this vital cellular process.

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