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Bioactivation, protein haptenation, and toxicity of sulfamethoxazole and dapsone in normal human dermal fibroblasts
Authors:Bhaiya Payal  Roychowdhury Sanjoy  Vyas Piyush M  Doll Mark A  Hein David W  Svensson Craig K
Affiliation:Division of Pharmaceutics, College of Pharmacy, The University of Iowa, Iowa City, IA 52242, USA.
Abstract:Cutaneous drug reactions (CDRs) associated with sulfonamides are believed to be mediated through the formation of reactive metabolites that result in cellular toxicity and protein haptenation. We evaluated the bioactivation and toxicity of sulfamethoxazole (SMX) and dapsone (DDS) in normal human dermal fibroblasts (NHDF). Incubation of cells with DDS or its metabolite (D-NOH) resulted in protein haptenation readily detected by confocal microscopy and ELISA. While the metabolite of SMX (S-NOH) haptenated intracellular proteins, adducts were not evident in incubations with SMX. Cells expressed abundant N-acetyltransferase-1 (NAT1) mRNA and activity, but little NAT2 mRNA or activity. Neither NAT1 nor NAT2 protein was detected. Incubation of NHDF with S-NOH or D-NOH increased reactive oxygen species formation and reduced glutathione content. NHDF were less susceptible to the cytotoxic effect of S-NOH and D-NOH than are keratinocytes. Our studies provide the novel observation that NHDF are able to acetylate both arylamine compounds and bioactivate the sulfone DDS, giving rise to haptenated proteins. The reactive metabolites of SMX and DDS also provoke oxidative stress in these cells in a time- and concentration-dependent fashion. Further work is needed to determine the role of the observed toxicity in mediating CDRs observed with these agents.
Keywords:AA  ascorbic acid  CDRs  cutaneous drug reactions  DDS  dapsone  D-NOH  dapsone hydroxylamine  ELISA  enzyme-linked immunosorbant assay  GSH  glutathione  HPLC  high performance liquid chromatography  NAT  N-acetyltransferase  NHEK  normal human epidermal keratinocytes  NHDF  normal human dermal fibroblasts  PABA  p-aminobenzoic acid  PBS  phosphate-buffered saline  ROS  reactive oxygen species  SMX  sulfamethoxazole  SMZ  sulfamethazine  S-NOH  sulfamethoxazole hydroxylamine
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