Date published: 2025-10-11

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Smac Inhibitors

The class of Smac inhibitors, as conceptualized in the table above, is characterized by their indirect action on the pathways and processes where Smac is involved. Smac functions as a pro-apoptotic factor by antagonizing IAPs. The listed chemicals modulate various aspects of the apoptotic pathways and related cellular processes, thereby influencing the role or necessity of Smac in these pathways. Most of these compounds work by either enhancing apoptosis through alternative pathways or modulating cellular survival signaling, which can reduce the reliance on Smac-mediated mechanisms. For instance, compounds like Z-VAD-FMK and Venetoclax modulate the balance between apoptotic and anti-apoptotic signaling, diminishing the need for Smac in the apoptosis process. Similarly, inhibitors of key signaling molecules such as NF-κB, PI3K, mTOR, and JAK2, like BAY 11-7082, LY294002, Rapamycin, and Ruxolitinib, respectively, alter the cellular signaling dynamics, affecting the role of Smac in these pathways.

Other compounds, including HSP90 inhibitor (17-AAG) and the proteasome inhibitor (Bortezomib), affect the stability and degradation of proteins involved in cell growth and survival. By modulating these processes, they can indirectly influence the functional significance of Smac in apoptosis. HDAC inhibitors like Vorinostat, which alter gene expression patterns, and PARP inhibitors like Olaparib, which affect DNA repair mechanisms, also contribute to this class by modulating cellular pathways that can indirectly reduce the reliance on Smac-mediated apoptosis. In summary, Smac inhibitors, as defined here, consist of a range of compounds that indirectly affect Smac's activity by influencing cellular pathways and processes related to apoptosis. These inhibitors do not target Smac directly but modulate the cellular environment and signaling pathways, thereby affecting the functional role or necessity of Smac in the apoptotic processes.

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