Abstract

Hypochlorous acid (HOCl) is a highly reactive product generated by the myeloperoxidase reaction during the oxidative burst of activated neutrophils, which is implicated in many bactericidal and cytotoxic responses. Recent evidence suggests that HOCl may also play a role in the modulation of redox sensitive signaling pathways. The short half-life of HOCl and the requirement for a continuous presence of H2O2 as a substrate for its myeloperoxidase-catalyzed generation make the study of HOCl-mediated responses very difficult. We describe here an enzymatic model consisting of glucose/glucose oxidase, catalase, and myeloperoxidase (GOX/CAT/MPO) that allows the controlled generation of both HOCl and H2O2 and thus, mimics the oxidative burst of activated neutrophils. By employing this model we show that HOCl prevents the H2O2-mediated activation of iron regulatory protein 1 (IRP1), a central post-transcriptional regulator of mammalian iron metabolism. Activated IRP1 binds to (R)iron-responsive elements" (IREs) within the mRNAs encoding proteins of iron metabolism and thereby controls their translation or stability. The inhibitory effect of HOCl is not a result of a direct modification of IRP1 by this oxidant. Kinetics experiments provide evidence that HOCl intervenes with the signaling cascade, which results in the activation of IRP1. We further demonstrate that HOCl antagonizes the H2O2-mediated increase in the levels of transferrin receptor, which is a downstream target of IRP1. Our findings suggest that HOCl can modulate signaling pathways in a concerted action with H2O2. The GOX/CAT/MPO system provides a valuable tool for studying the regulatory function of HOCl.

Highlights

  • Phagocytic cells, including neutrophils and macrophages, have an important function in the inflammatory response

  • By employing this model we show that hypochlorous acid (HOCl) prevents the H2O2-mediated activation of iron regulatory protein 1 (IRP1), a central post-transcriptional regulator of mammalian iron metabolism

  • We further demonstrate that HOCl antagonizes the H2O2-mediated increase in the levels of transferrin receptor, which is a downstream target of IRP1

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Summary

Introduction

Phagocytic cells, including neutrophils and macrophages, have an important function in the inflammatory response. Exposure of mammalian cells or tissues to H2O2 results in activation of iron regulatory protein 1 (IRP1) (24 –27), a central posttranscriptional regulator of cellular iron metabolism (28, 29). The mechanism does not involve a direct attack of the iron-sulfur cluster by H2O2, and a mere increase in intracellular H2O2 levels is not sufficient to activate IRP1 (27). The well-established role of iron and H2O2 in tissue injury (31), based on Fenton chemistry, e.g. the iron-catalyzed decomposition of H2O2 to aggressive hydroxyl radicals, suggests that this response may have important pathophysiological implications This is relevant in inflammation, where cytotoxic immune cells release large amounts of reactive oxygen species. In stimulated neutrophils the release of H2O2 can increase by a factor of 10 and reach micromolar concentrations (26)

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