Date published: 2025-9-19

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Hrs-2 Inhibitors

Chemical inhibitors of Hrs-2 target various aspects of the protein's role in endocytic trafficking and endosome function. Benzyl isothiocyanate can inhibit Hrs-2 by covalently modifying cysteine residues, a process that can disrupt the protein's structural integrity and function in endosomal cargo sorting. Similarly, agents that alter endosomal pH, such as Chloroquine, undermine the acidic environment critical for Hrs-2's activity in sorting endocytosed materials. Monensin, an ionophore, disrupts endosomal ion gradients, further impeding Hrs-2's ability to facilitate correct cargo trafficking within endosomes. Bafilomycin A1 also targets the acidification process by inhibiting the V-ATPase proton pump, which could prevent the endosomal sorting of molecules dependent on Hrs-2.

Additional inhibitors, like Dynasore, interfere with the endocytosis process itself by targeting dynamin, which is essential for vesicle scission from the plasma membrane and could indirectly inhibit Hrs-2's subsequent endosomal functions. Similarly, Pitstop 2 blocks clathrin-mediated endocytosis, a pathway that feeds into the endosomal sorting role of Hrs-2. Compounds like Itraconazole and Methyl-β-cyclodextrin, which disrupt endosomal cholesterol homeostasis, can also inhibit Hrs-2 by altering the lipid composition of endosomal membranes and potentially disrupting lipid rafts that are crucial for Hrs-2's function. Filipin III binds to cholesterol, which can disturb the membrane domains where Hrs-2 operates. Genistein, a tyrosine kinase inhibitor, can block phosphorylation events that might be necessary for Hrs-2-mediated signaling and trafficking interactions. Disruptive agents like Nocodazole and Cytochalasin D, which interfere with microtubules and actin filaments respectively, can inhibit Hrs-2 by preventing the proper positioning and movement of endosomes within the cell, thereby impeding the protein's role in the endosomal sorting process.

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