Date published: 2025-9-13

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Nth2 Inhibitors

Chemical inhibitors of Nth2 can exert their inhibitory effects through various interactions with the protein itself or its DNA substrates. Resveratrol can inhibit Nth2 by binding directly to DNA, altering its structure and impeding the access of Nth2 to oxidative DNA lesions that it is responsible for repairing. Similarly, Curcumin can compete with Nth2 for DNA binding, thus obstructing its ability to recognize and repair damaged DNA. Metals such as Zinc Chloride and Cadmium Chloride can interfere with the DNA repair activity of Nth2 through binding interactions that either alter the enzyme's structure or compete with the DNA substrate, which is crucial for the enzyme's function. Hesperidin contributes to the inhibition of Nth2 by reducing oxidative stress, thereby decreasing the occurrence of the DNA lesions that Nth2 would typically repair.

Other plant-derived polyphenols like Ellagic Acid, Epigallocatechin Gallate (EGCG), and Quercetin can also inhibit Nth2 by directly interacting with the DNA substrate or the enzyme itself. Ellagic Acid's binding to DNA can block the association of Nth2 with its substrates, hindering its base excision repair mechanism. EGCG and Quercetin can bind to Nth2 or DNA, altering the enzyme's capacity to interact with and repair damaged DNA. Genistein, with its DNA mimicry properties, can bind to Nth2 or its DNA substrates, disrupting the protein's normal function in the DNA repair process. Caffeic Acid and Chlorogenic Acid employ a different strategy by forming adducts with DNA, which could prevent Nth2 from accessing and fixing DNA lesions. Chlorogenic Acid also acts as an antioxidant, potentially altering the oxidative environment in which Nth2 operates. Lastly, Auranofin targets the cellular redox balance by binding to thioredoxin reductase, an enzyme that maintains the redox state that Nth2 relies on for proper function, thus indirectly inhibiting the DNA repair activity of Nth2.

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