Date published: 2025-9-17

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Ran BP-2 Inhibitors

Ran BP-2 inhibitors encompass a variety of compounds that can either directly or indirectly inhibit the activity of Ran BP-2, a critical regulator of nucleocytoplasmic transport and cellular processes. These inhibitors exert their effects through different mechanisms, primarily by disrupting Ran BP-2 interactions, post-translational modifications, or cellular pathways. Direct inhibitors like Importazole interfere with the specific binding between Ran BP-2 and importin β, preventing the translocation of cargo proteins into the nucleus. Meanwhile, indirect inhibitors such as MLN4924 target the neddylation pathway, destabilizing cullin-RING ligases (CRLs) that regulate Ran BP-2 levels. Leptomycin B, on the other hand, indirectly inhibits Ran BP-2 by blocking CRM1-mediated nuclear export, leading to nuclear retention. Additionally, compounds like Ranolazine and Gefitinib influence Ran BP-2 by affecting intracellular calcium levels or the EGFR pathway, respectively.

Nutlin-3 disrupts the interaction between MDM2 and p53, resulting in altered Ran BP-2 expression and localization. KPT-185 and Actinomycin D indirectly inhibit Ran BP-2 by interfering with nucleocytoplasmic transport processes. Geldanamycin binds to Hsp90, causing Ran BP-2 degradation. MK-2206 modulates Ran BP-2 through Akt inhibition, and WP1130 induces proteasomal degradation of Ran BP-2 by targeting USP9X. Methotrexate interferes with the folate pathway, affecting nucleocytoplasmic transport and Ran BP-2 function. These diverse inhibitors provide valuable tools for investigating the intricate regulation of Ran BP-2 and its impact on cellular processes.

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