The chemical inhibitors listed aim to affect ISOC2 functionality based on its involvement in protein destabilization and its cytoplasmic and nuclear localization. Proteasome inhibitors such as MG-132, for example, inhibit the breakdown of proteins, which could counteract the protein-destabilizing function of ISOC2. On the other hand, inhibitors like Nocodazole and Leptomycin B traps ISOC2 in specific cellular compartments, thus affecting its ability to destabilize proteins.
Another category of inhibitors focuses on broader cellular signaling pathways related to protein stability. In this context, kinase inhibitors like Staurosporine, Wortmannin, and LY294002 can inhibit proteins that play a role in protein stability and turnover. These inhibitors affect downstream signaling pathways, such as those mediated by PKC, PI3K, and mTOR, that could indirectly affect ISOC2's function. By targeting these signaling nodes, the homeostatic balance of protein stability and degradation within the cell could be shifted, thereby affecting the functional role of ISOC2 in these processes.
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