Date published: 2025-9-22

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4933437F05Rik Inhibitors

Noxred1 Inhibitors span a range of compounds that have the capacity to alter the activity of NADP+ dependent oxidoreductase domain containing 1 indirectly through modulation of redox states and related signaling pathways. Diphenyleneiodonium chloride, a nonspecific inhibitor, can disrupt electron transport chains that Noxred1 may be part of, while Apocynin can prevent the proper assembly of NADPH oxidase complexes, which could limit the availability of NADPH for Noxred1. The action of Allopurinol could lead to increased NADPH levels by inhibiting xanthine oxidase, thus affecting the redox balance that Noxred1 might be regulating.

Compounds such as Quercetin and Genistein, known to inhibit kinases and reductases, can alter signaling pathways and the cellular redox environment, both of which are essential for Noxred1 function. Curcumin and Resveratrol, through their antioxidant effects, might change the redox state of cells, potentially impacting the function of redox-sensitive enzymes like Noxred1. FAD, as a cofactor, can competitively bind to enzymes using similar cofactors, which could influence Noxred1 activity. N-acetyl cysteine, by boosting glutathione levels, can shift the redox balance in cells, thereby possibly affecting Noxred1's role in redox reactions. Methylene blue acts as a redox cycling agent and, in doing so, could perturb the redox dynamics that Noxred1 is involved in maintaining. Ellagic acid and Rutin, through their influence on oxidative processes, can modulate the activity of enzymes participating in redox homeostasis, such as Noxred1.

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