Date published: 2025-10-13

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Gm221 Inhibitors

The class of compounds labeled as Ccdc170 Inhibitors includes a variety of chemicals that target different cellular processes and signaling pathways, which can indirectly impact the function of CCDC170. For instance, Rapamycin and Wortmannin are known to inhibit mTOR and PI3K respectively, pathways that orchestrate cell growth and survival, possibly affecting the synthesis or downstream effects of CCDC170. Inhibitors of the MAPK signaling cascade, such as PD98059 and SB203580, can alter cellular responses to various stimuli, which may impinge upon the regulatory roles of CCDC170.

Proteasome inhibitors like Bortezomib and MG132 can lead to the accumulation of proteins within the cell due to impaired degradation, which in turn could affect the levels and activity of CCDC170. Cycloheximide's inhibition of protein synthesis is a more direct approach that can result in decreased expression of rapidly turned over proteins, including potentially CCDC170. The inhibition of molecular chaperones, such as with 17-AAG, can disrupt protein folding and stability, influencing the functional state of CCDC170. Additionally, compounds like Y-27632 target the Rho kinase pathway, which is integral to cytoskeletal dynamics and cellular architecture. Such alterations in the cellular framework can influence the context in which CCDC170 operates, affecting its functional interactions. Each of these inhibitors, while not directly targeting CCDC170, can manipulate cellular systems and mechanisms that are crucial to CCDC170's role within the cell.

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