Date published: 2025-10-11

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C9orf9 Inhibitors

Staurosporine is known for its broad-spectrum kinase inhibition, potentially affecting numerous signaling cascades that regulate proteins like C9orf9. On the other hand, compounds such as Trichostatin A and Sodium Butyrate exert their effects on gene expression by inhibiting histone deacetylases, thereby potentially altering the chromatin dynamics and the transcriptional landscape within which C9orf9 operates. Furthermore, proteasome inhibitors like MG132 can impact the degradation pathways of intracellular proteins, possibly influencing the stability and abundance of C9orf9. Similarly, PD98059's inhibition of the MEK enzyme, LY294002's interference with the PI3K/AKT pathway, and Rapamycin's suppression of mTOR all serve to modulate key regulatory pathways that have the potential to govern the function and expression of C9orf9.

Additionally, KN-93's role in inhibiting calcium/calmodulin-dependent protein kinase II, and SB431542's targeting of TGF-β receptor kinases, illustrates the diversity of signaling molecules whose modulation might impact C9orf9's activity. Compounds like QNZ also participate in the regulation of inflammatory and immune pathways and could, therefore, influence responses in which C9orf9 is implicated. JNK inhibitors like SP600125 have the capacity to alter stress response and apoptotic signaling, pathways that could intersect with the biological role of C9orf9.

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