The chemical class known as IκB-ε Inhibitors encompasses a range of compounds that, while not directly targeting IκB-ε, exert their inhibitory effects through the modulation of various signaling pathways that are integral to the function of IκB-ε. These compounds achieve this by targeting different aspects of the NF-κB pathway or related cellular processes. For instance, inhibitors like BAY 11-7082 and IKK-16 focus on preventing the activation of NF-κB by inhibiting the phosphorylation and degradation of IκB proteins, including IκB-ε. On the other hand, proteasome inhibitors like Bortezomib hinder the degradation process of phosphorylated IκB-ε, thus influencing its function in the NF-κB signaling pathway.
Additionally, compounds such as SP600125, SB203580, and PD98059 target various MAP kinases, which play a pivotal role in signaling cascades that intersect with NF-κB pathways. The modulation of these kinases indirectly impacts IκB-ε's role in NF-κB signaling. Other compounds like Hydroxychloroquine and Anakinra influence NF-κB activity through their effects on Toll-like receptor and cytokine signaling, respectively. Reactive oxygen species inhibitors like N-acetylcysteine and calcium signaling modulators like Verapamil also play a role in indirectly influencing the function of IκB-ε.
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