InAADR

Protein Information

Protein Name: Glutathione reductase (P00390)
Gene Name: GSR
Description: Glutathione reductase, mitochondrial precursor (EC 1 8 1 7) (GR) (GRase)
PDB ID: 1ALG
Protein Family:
Protein Category: Enzyme

This panel provides drug-protein interaction and their ADRs along with references

Interacting Drugs Toxicity Mechanism Reference
Cisplatin Ototoxicity Cisplatin ototoxicity is related to depletion of glutathione and glutathione reductase in the cochlea [ ADR Type 2 ] Application of antioxidants and other agents to prevent cisplatin ototoxicity
Cyclophosphamide Lung Toxicity Significant reductions (P less than 0 005) in G6PD, GSH-R, and GSH-P activities occurred on days 1-5,indicating that Cyclophosphamide causes lung toxicity [ ADR Type 2 ] Cyclophosphamide-induced depression of the antioxidant defense mechanisms of the lung
Epinephrine Cytotoxicity Pretreatment of cells with 100 microM 1,3-bis(2-chloroethyl)-1-nitrosourea which inhibits glutathione reductase,increased the sensitivity of these cells to the epinephrine plasma,which was found to be cytotoxic when incubated with isolated heart cells. [ ADR Type 1 ] Epinephrine-induced cytotoxicity of rat plasma Its effects on isolated cardiac myocytes Lab
Ketoprofen Intestinal Toxicity A significant increase of tumor necrosis factor-alpha production and decreases in glutathione levels and glutathione reductase activity after treatment of the racemate and (R)-(-)-ketoprofen,suggesting induced intestinal toxicity could be correlated with a reduced oxidative damage characterized not only by a lack of changes in glutathione reductase activity but also by an absence of up-regulation of tumor necrosis factor-alpha production in intestinal mucosa. [ ADR Type 2 ] Mechanisms involved in the attenuation of intestinal toxicity induced by (S)-(+)-ketoprofen in re-fed rats

This panel provides information on drug category

Toxicity Source

InAADR: Drug-Protein-ADRs database