Date published: 2025-9-15

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VMA21 Inhibitors

The chemical class VMA21 Inhibitors is a conceptual category comprising compounds that can indirectly influence the activity of the VMA21 protein. Given that VMA21 is involved in the assembly of the V-ATPase complex, chemicals that affect the V-ATPase or the acidification of organelles where this complex operates can, in turn, modulate the function of VMA21. These inhibitors do not directly target VMA21 itself but impact the cellular environment or the components that VMA21 interacts with, thereby altering its function.

Bafilomycin A1 and concanamycin A are V-ATPase inhibitors, and by hindering V-ATPase activity, they can indirectly affect the role of VMA21 in the assembly and functioning of this complex. Similarly, chloroquine and hydroxychloroquine, known for their ability to elevate the pH of endosomes and lysosomes, can alter the environment necessary for optimal V-ATPase function, thereby impacting VMA21's role in the process. Saliphenylhalamide, although lacking a CAS number, is also known to inhibit V-ATPase, suggesting a similar mode of indirect influence on VMA21. Other compounds like enoxacin, mebendazole, monensin, and ionomycin have distinct primary targets but can also affect the endosomal-lysosomal system or intracellular calcium homeostasis, which are critical factors for the proper functioning of the V-ATPase complex and, by extension, VMA21's role therein. Niclosamide disrupts ATP production, affecting energy-dependent processes including those mediated by VMA21. Proton pump inhibitors like omeprazole and drugs like zoledronic acid that affect osteoclast function exemplify the diversity of mechanisms by which VMA21 activity can be indirectly influenced through modulation of cellular acidification and V-ATPase function. These chemicals thus represent indirect methods of modulating VMA21 activity by targeting broader cellular systems and processes that are essential for its functional expression within the cell.

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