Date published: 2025-10-11

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Ninein Inhibitors

Ninein, a centrosomal protein critical for microtubule anchoring and organization, can be modulated by a diverse array of chemical inhibitors. These inhibitors target various cellular pathways and molecular players, exerting their effects through both direct and indirect mechanisms. One such class of inhibitors includes mitotic disruptors like Vinblastine and RO-3306. Vinblastine interferes with microtubule dynamics, disrupting Ninein's role in microtubule organization. RO-3306, a selective CDK1 inhibitor, impacts cell cycle progression, influencing Ninein during mitotic events. Another set of inhibitors focuses on kinases associated with Ninein-related signaling pathways. For instance, GW441756 targets c-Met kinase, influencing Ninein through shared cellular pathways. LY294002, an inhibitor of PI3-kinase, affects downstream signaling events, indirectly modulating Ninein functions. Additionally, BI2536, a PLK1 inhibitor, can impact microtubule dynamics and Ninein-associated processes.

Beyond kinase inhibitors, compounds like Ciliobrevin A disrupt primary cilia formation, altering Ninein's cellular localization and function indirectly. Griseofulvin, by impeding microtubule assembly, further contributes to the modulation of Ninein's role in microtubule organization. Moreover, AZD7762, a Chk1 inhibitor, influences cell cycle progression, impacting Ninein-associated cellular events. In summary, the class of Ninein inhibitors comprises diverse chemicals targeting key cellular pathways and molecular processes. These inhibitors, ranging from mitotic disruptors to kinase inhibitors, provide a toolbox for researchers investigating Ninein's intricate regulatory network. Understanding the specific biochemical and cellular pathways influenced by each inhibitor is crucial for unraveling the complex interplay of Ninein in cellular processes.

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