Date published: 2025-9-19

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ARMC9 Inhibitors

ARMC9 Inhibitors target various aspects of cellular processes such as ciliogenesis, centrosome function, and cell cycle regulation, potentially influencing the functional context of ARMC9. Given ARMC9's involvement in cilia-related pathways, modulation of these processes could indirectly impact its activity.Inhibitors of microtubule dynamics, such as Nocodazole, Colchicine, and Taxol, can affect centrosome and cilium stability, potentially impacting ARMC9's function in these structures. Cycloheximide's inhibition of protein synthesis and Trichloroacetaldehyde-13C2's effect on ciliary beating provide insights into how protein production and ciliary function can be modulated, potentially influencing ARMC9's role. Rapamycin's inhibition of mTOR and cyclin-dependent kinase inhibitors like Roscovitine and Alsterpaullone underscore the importance of cell growth, proliferation, and cell cycle regulation in the context of ciliogenesis, where ARMC9 might be involved. Lithium Chloride's impact on Wnt signaling and Forskolin's activation of adenylate cyclase highlight the role of signaling pathways in ciliary formation and function.

Additionally, Aurora kinase inhibitors like ZM-447439 and autophagy-related compounds like Bafilomycin A1 could also have implications for centrosome and cilium functions, indirectly influencing ARMC9. These compounds, while not directly targeting ARMC9, are important for exploring the complex processes of ciliogenesis, centrosome dynamics, and cellular signaling. They offer valuable tools for research into the roles of proteins involved in ciliary formation and function, with potential implications for understanding diseases related to ciliary dysfunction.

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