Date published: 2025-10-29

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8-hydroxyguanine Inhibitors

8-Hydroxyguanine Inhibitors are a specialized class of chemical compounds that target 8-hydroxyguanine, a common oxidative modification of guanine, one of the four primary nucleobases in DNA. 8-Hydroxyguanine (8-oxoG) results from oxidative stress and can cause significant damage to the genetic material by pairing incorrectly during DNA replication, leading to mutations. Inhibitors of 8-hydroxyguanine function by binding to either the modified guanine base itself or to enzymes involved in recognizing and processing 8-oxoG, thereby interfering with the pathways that handle this oxidative lesion. These inhibitors are designed to either prevent the incorporation of 8-oxoG into DNA or block the recognition and excision processes that typically repair this damaged base.

The chemical design of 8-Hydroxyguanine Inhibitors focuses on achieving high specificity and strong affinity for the 8-oxoG lesion or its associated enzymes. The structure of these inhibitors often includes aromatic or heterocyclic rings that can stack with the planar structure of 8-oxoG, enhancing binding through π-π interactions. Additionally, these inhibitors may contain functional groups capable of forming hydrogen bonds with key amino acids in the active site of repair enzymes, thereby stabilizing the inhibitor-enzyme complex. The physicochemical properties of these inhibitors, such as solubility, stability, and lipophilicity, are optimized to ensure effective interaction with 8-oxoG or its processing enzymes in the cellular environment. Moreover, the binding kinetics, including the rates of association and dissociation, are crucial factors that influence the efficacy of these inhibitors in modulating the recognition and repair of 8-oxoG. By studying the interactions between 8-Hydroxyguanine Inhibitors and their targets, researchers can gain a deeper understanding of the molecular mechanisms underlying oxidative DNA damage and the broader implications for genetic stability and cellular function.

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