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Merck

Sulfa drugs inhibit sepiapterin reduction and chemical redox cycling by sepiapterin reductase.

The Journal of pharmacology and experimental therapeutics (2015-01-01)
Shaojun Yang, Yi-Hua Jan, Vladimir Mishin, Jason R Richardson, Muhammad M Hossain, Ned D Heindel, Diane E Heck, Debra L Laskin, Jeffrey D Laskin
ABSTRAKT

Sepiapterin reductase (SPR) catalyzes the reduction of sepiapterin to dihydrobiopterin (BH2), the precursor for tetrahydrobiopterin (BH4), a cofactor critical for nitric oxide biosynthesis and alkylglycerol and aromatic amino acid metabolism. SPR also mediates chemical redox cycling, catalyzing one-electron reduction of redox-active chemicals, including quinones and bipyridinium herbicides (e.g., menadione, 9,10-phenanthrenequinone, and diquat); rapid reaction of the reduced radicals with molecular oxygen generates reactive oxygen species (ROS). Using recombinant human SPR, sulfonamide- and sulfonylurea-based sulfa drugs were found to be potent noncompetitive inhibitors of both sepiapterin reduction and redox cycling. The most potent inhibitors of sepiapterin reduction (IC50s = 31-180 nM) were sulfasalazine, sulfathiazole, sulfapyridine, sulfamethoxazole, and chlorpropamide. Higher concentrations of the sulfa drugs (IC50s = 0.37-19.4 μM) were required to inhibit redox cycling, presumably because of distinct mechanisms of sepiapterin reduction and redox cycling. In PC12 cells, which generate catecholamine and monoamine neurotransmitters via BH4-dependent amino acid hydroxylases, sulfa drugs inhibited both BH2/BH4 biosynthesis and redox cycling mediated by SPR. Inhibition of BH2/BH4 resulted in decreased production of dopamine and dopamine metabolites, 3,4-dihydroxyphenylacetic acid and homovanillic acid, and 5-hydroxytryptamine. Sulfathiazole (200 μM) markedly suppressed neurotransmitter production, an effect reversed by BH4. These data suggest that SPR and BH4-dependent enzymes, are "off-targets" of sulfa drugs, which may underlie their untoward effects. The ability of the sulfa drugs to inhibit redox cycling may ameliorate ROS-mediated toxicity generated by redox active drugs and chemicals, contributing to their anti-inflammatory activity.

MATERIAŁY
Numer produktu
Marka
Opis produktu

Supelco
Sulfapyridine melting point standard, Pharmaceutical Secondary Standard; Certified Reference Material
Supelco
Sulfathiazole, VETRANAL®, analytical standard
Sigma-Aldrich
9,10-Phenanthrenequinone, ≥99%
Sigma-Aldrich
9,10-Phenanthrenequinone, 95%
Supelco
Menadione (K3), analytical standard
Supelco
Sulfamethoxazole, VETRANAL®, analytical standard
Supelco
Sulfapyridine, VETRANAL®, analytical standard
Supelco
Sulfamethoxazole, certified reference material, TraceCERT®, Manufactured by: Sigma-Aldrich Production GmbH, Switzerland
Menadione, European Pharmacopoeia (EP) Reference Standard
USP
Sulfamethoxazole, United States Pharmacopeia (USP) Reference Standard
Chlorpropamide, European Pharmacopoeia (EP) Reference Standard
Supelco
Sulfamethoxazole, Pharmaceutical Secondary Standard; Certified Reference Material
Supelco
Menadione, Pharmaceutical Secondary Standard; Certified Reference Material
USP
Menadione, United States Pharmacopeia (USP) Reference Standard
Sulfamethoxazole, European Pharmacopoeia (EP) Reference Standard
Sulfathiazole, European Pharmacopoeia (EP) Reference Standard
Tolbutamide, European Pharmacopoeia (EP) Reference Standard
Sulfapyridine, European Pharmacopoeia (EP) Reference Standard
Sigma-Aldrich
Menadione, meets USP testing specifications
Supelco
Sulfathiazole
Sigma-Aldrich
Sulfasalazine, 97.0-101.5%
Sigma-Aldrich
Menadione, crystalline
Supelco
Sulfapyridine, ≥99.0%
Supelco
Chlorpropamide, analytical standard, ≥97%
Supelco
Sulfamethoxazole
Supelco
Tolbutamide, analytical standard