2B28 inhibitors are chemicals that indirectly disrupt the function of 2B28 by modulating various cellular pathways involved in protein degradation. Staurosporine, for example, targets protein kinase C (PKC) and by doing so, can impair the NF-κB pathway, which is crucial for the transcription of several proteins that are substrates for the 2B28 protein. This inhibition could decrease the pool of proteins requiring ubiquitin-mediated degradation, reducing the functional demand on 2B28.
Similarly, compounds like LY294002 that inhibit the PI3K/AKT pathway can lead to a general reduction in protein turnover. Since 2B28 is involved in the tagging of proteins for degradation, a reduction in protein turnover implies that there are fewer proteins requiring the attention of 2B28, leading to a decrease in its activity. Proteasome inhibitors, such as MG-132, Bortezomib, Epoxomicin, Lactacystin, and Omuralide, directly block the degradation of ubiquitinated proteins. This can lead to an accumulation of proteins within the cell, potentially causing a feedback effect that reduces the activity of components like 2B28 that are upstream in the ubiquitination pathway.
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