Chemical inhibitors of GSTT2B can be characterized by their ability to interfere with the enzyme's glutathione-conjugating activity. Ethacrynic acid, for instance, covalently modifies cysteine residues within the active site of GSTT2B, which diminishes the enzyme's capacity to catalyze the conjugation of glutathione to its substrates. Similarly, Cibacron Blue 3GA acts by occupying the active site of GSTT2B, effectively mimicking the substrate and preventing actual substrates from binding, thereby inhibiting the enzyme's function. Hematin targets the heme group associated with the GST family, inducing a conformational change that results in reduced enzymatic activity. Curcumin, known for its electrophilic nature, can react with nucleophilic centers on GSTT2B, leading to structural and functional modifications. Ellagic acid targets the G-site of GSTT2B, preventing glutathione binding and thus the detoxification process that the enzyme catalyzes.
Continuing with the array of chemical inhibitors, Sulfasalazine serves as a competitive inhibitor by binding to the active site of GSTT2B, displacing glutathione. Menadione induces the production of reactive oxygen species through redox cycling, which in turn can modify the active-site thiol groups of GSTT2B, leading to inhibition. Parthenolide forms adducts with cysteine residues in the enzyme's active site, hindering its function. Chrysin and capsaicin inhibit GSTT2B by competing for the active site, obstructing substrate and glutathione access. Phenethyl isothiocyanate can react with amino acid residues essential for GSTT2B activity, particularly modifying lysine residues, which results in inhibition. Lastly, tetraethylthiuram disulfide inhibits GSTT2B by binding to thiol groups of glutathione, thus reducing its availability for conjugation reactions that GSTT2B facilitates, leading to a decrease in the enzyme's activity. Each of these chemicals disrupts the normal function of GSTT2B through a unique mechanism that directly compromises its ability to catalyze the glutathione conjugation reactions.
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