Date published: 2025-9-19

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FAM179A Inhibitors

FAM179A inhibitors encompass a range of compounds that indirectly influence the protein by modulating cellular signaling pathways and processes. Staurosporine and LY294002 exemplify this by targeting kinase activity and PI3K/Akt signaling, respectively. These pathways are pivotal in regulating protein functions within the cell, and by inhibiting them, the compounds indirectly affect the regulation and function of FAM179A. Compounds such as U0126 and PD98059 focus on the MAPK/ERK pathway, while SP600125 and SB203580 target the JNK and p38 MAPK pathways. Disruption of these pathways by these inhibitors can lead to altered cellular responses and indirectly modulate the activity or expression of FAM179A.

Rapamycin is another agent that intervenes by inhibiting the mTOR pathway, crucial for protein synthesis. By impeding this pathway, FAM179A synthesis may be reduced. Wortmannin is also involved in this pathway, acting on PI3K and leading to similar downstream effects. Beyond signaling, inhibitors like Cycloheximide and Actinomycin D attack the core processes of protein synthesis and gene transcription. By halting these fundamental cellular mechanisms, the production of FAM179A can be curtailed. In contrast, Bortezomib and MG132 target the proteasome, a complex responsible for protein degradation. Inhibition of the proteasome can lead to an accumulation of proteins, which may alter the degradation dynamics of FAM179A, affecting its cellular concentration.

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