Date published: 2025-12-23

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Gm962 Inhibitors

The chemical class termed Ap5b1 Inhibitors encompasses a range of compounds that indirectly influence the function of the adaptor-related protein complex 5, beta 1 subunit (Ap5b1). These compounds act by altering various cellular mechanisms and processes that are essential for the proper functioning of Ap5b1. Ionophores such as Monensin disrupt the ionic balance within the Golgi, which can indirectly affect the operation of Ap5b1 by changing the environment it requires to function effectively. Inhibitors of vesicular acidification like Bafilomycin A1 and Chloroquine hamper endosomal sorting, an essential process in which Ap5b1 is implicated, thereby impacting its ability to sort cargo molecules.

Additionally, compounds that affect the cytoskeletal elements and vesicle formation processes, such as Nocodazole, Cytochalasin D, Vinblastine, and Paclitaxel, can inhibit Ap5b1 by interfering with the physical structures required for vesicle movement and cargo transport. These agents lead to the disruption of microtubules or actin filaments, which are crucial for the intracellular transport that Ap5b1 facilitates. Small molecule inhibitors such as Wortmannin and Genistein that target signaling pathways, specifically those involving PI3K and tyrosine kinases, can inhibit Ap5b1 by modifying the signaling cascades that regulate vesicular trafficking. Pitstop 2 and Endosidin2 represent other classes of inhibitors that obstruct clathrin-mediated endocytosis and endosomal trafficking, respectively, demonstrating the broad spectrum of mechanisms through which these compounds can indirectly inhibit Ap5b1.

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