Date published: 2025-10-12

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C9orf47 Inhibitors

PD98059 and SB203580 target the MAPK signaling pathway at different points, which is essential for cell differentiation, proliferation, and stress responses. By influencing this pathway, the activity of C9orf47 can be indirectly modulated. PI3K inhibitors, LY294002 and Wortmannin, play a role in the AKT signaling pathway, which is critical for cell survival. The inhibition of PI3K can disrupt the balance of survival signals, affecting proteins associated with this pathway, including potentially C9orf47. NF449, by inhibiting G-protein signaling, can alter the levels of cyclic AMP, a pivotal second messenger in a variety of signaling pathways, thus potentially impacting C9orf47's regulation.

Erlotinib and Sorafenib are tyrosine kinase inhibitors that target EGFR and multiple kinases, respectively. These enzymes are key regulators of cell growth and survival signaling pathways. By inhibiting these kinases, the compounds can alter the signaling cascades that might intersect with C9orf47's function. PD173074's inhibition of FGFR tyrosine kinase can similarly change growth factor signaling, potentially affecting C9orf47. ZM-447439 and Y-27632 target cell cycle progression and cell morphology by inhibiting Aurora kinase and ROCK kinase, respectively. These processes are crucial for normal cell division and structural integrity, and their inhibition can indirectly influence proteins involved in these processes. KN-93's inhibition of CaMKII affects calcium signaling, which is important in many cellular functions, including those that might be regulated by C9orf47. 2-Methoxyestradiol disrupts HIF-1alpha and microtubule function, which can impact cellular responses to hypoxia and cell division, thereby potentially affecting C9orf47's activity.

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