Date published: 2025-10-12

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FAM111A Inhibitors

FAM111A inhibitors, as tabulated, constitute chemicals that primarily operate indirectly to modulate the functional context or stability of FAM111A. These chemicals primarily target cellular pathways or processes that FAM111A might be associated with, albeit indirectly. Roscovitine, for example, is a potent inhibitor of cyclin-dependent kinases which are key regulatory enzymes in the cell cycle. Its inhibitory action can influence cell cycle progression, and proteins like FAM111A which may play roles in this process might thus be affected. Similarly, Paclitaxel stabilizes microtubules, which are pivotal for cell division. Any role FAM111A has in cell division or associated processes would be influenced in cells with this agent.

Furthermore, MG-132 operates by inhibiting the proteasome, a complex responsible for degrading unwanted or damaged proteins. Through this action, MG-132 can indirectly influence the stability of FAM111A. On the other hand, agents like 5-Fluorouracil, Nocodazole, and Mitomycin C are deeply intertwined with DNA metabolism and mitotic processes, presenting avenues through which they might influence FAM111A. Finally, the remainder of the listed chemicals, including Rapamycin, Chloroquine, and the kinase inhibitors, provide a broad-spectrum approach, targeting central cellular pathways which, when modulated, can indirectly affect the function or context of FAM111A within the cell.

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