Date published: 2025-9-17

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ZDHHC7 Inhibitors

The chemical class known as ZDHHC7 Inhibitors encompasses a diverse array of compounds that interact with and influence the ZDHHC7 protein through indirect mechanisms. ZDHHC7, involved in the palmitoylation process, plays a crucial role in the post-translational modification of proteins. This class includes inhibitors that target the biochemical pathways and processes central to palmitoylation, thereby exerting an influence over ZDHHC7's function. For instance, 2-Bromopalmitate, by inhibiting protein palmitoylation, disrupts the very process that ZDHHC7 mediates. This interference with palmitoylation directly impacts the functional capacity of ZDHHC7 in cellular processes. Similarly, compounds like Tunicamycin and Cerulenin, which inhibit N-linked glycosylation and fatty acid synthesis respectively, affect the substrate availability and processing dynamics critical to ZDHHC7's activity. These inhibitors, by altering the availability of palmitic acid and the folding of protein substrates, influence ZDHHC7's role in cellular protein modification.

Moreover, the class includes a range of HMG-CoA reductase inhibitors like PF-6463922, Fluvastatin, Simvastatin, Lovastatin, Atorvastatin, and Mevastatin. These inhibitors, by impacting lipid metabolism and cholesterol biosynthesis, indirectly influence the palmitoylation process. Their action on lipid metabolism affects the availability of substrates necessary for the function of ZDHHC7, thereby modulating its activity. Triacsin C, another key member of this class, inhibits acyl-CoA synthetase, further reducing the fatty acid availability for palmitoylation, thereby impacting ZDHHC7's function. Additionally, Curcumin, through its modulation of various cellular pathways including lipid metabolism, influences the broader cellular environment in which ZDHHC7 operates. Fenofibrate, as a PPARα agonist, also contributes to this modulation by affecting lipid metabolism pathways, thereby influencing the activity of ZDHHC7.

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