IL-4 gene expression up-regulated by mercury in rat mast cells: a role of oxidant stress in IL-4 transcription

doi:10.1093/intimm/13.3.297

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International Immunology, Vol. 13, No. 3, 297-304, March 2001
© 2001 Japanese Society for Immunology

IL-4 gene expression up-regulated by mercury in rat mast cells: a role of oxidant stress in IL-4 transcription

Zhonglin Wu, David R. Turner¹^, and David B. G. Oliveira

Divisions of Renal Medicine and
¹ Histopathology, St George's Hospital Medical School, Cranmer Terrace, London SW17 0RE, UK

Correspondence to: Z. Wu

In the Brown Norway (BN) rat, chemical compounds [mercuric chloride(HgCl₂), D-penicillamine or gold salts] induce a T_h2-dominatedautoimmune syndrome with tissue injury in the form of a vasculitisand arthritis. An early phase of vasculitis in the model occurswithin 24 h of an injection of HgCl₂, is ${alpha}$ ß T cellindependent and involves the mast cell. In addition, HgCl₂ inducesIL-4 mRNA in mast cells from BN rats. Our recent work has demonstratedthat the balance of oxidative/antioxidative influences playsan important role in the modulation of mast cell function (degranulation)in chemically induced autoimmunity. The aim of this study wasto determine, in mast cells, whether oxidative status influencesIL-4 transcription and translation, which is required for thedevelopment of a T_h2 response. Exposure of the mast cell lineRBL-2H3 to HgCl₂ enhanced both IL-4 mRNA and its promoter activity.Oxidative stress by hydrogen peroxide mimicked the effects ofHgCl₂ in enhancing IL-4 promoter activity. The enhancement ofIL-4 gene expression by HgCl₂ was significantly reduced by antioxidants(both sulphydryl and non-sulphydryl containing). The same patternof regulation was also observed on IL-4 protein expression inthe mast cells. These data suggest a novel mechanism of IL-4transcriptional up-regulation by oxidative stress. Our resultsprovide evidence to support our hypothesis that alterationsin intracellular reactive oxygen species production modulateboth IL-4 gene expression and mast cell function.

Keywords: IL-4, mast cells, oxidant stress

Transmitting editor: M. Feldmann

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