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2-thioxanthines are mechanism-based inactivators of myeloperoxidase that block oxidative stress during inflammation |
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| Authors: | Tidén Anna-Karin Sjögren Tove Svensson Mats Bernlind Alexandra Senthilmohan Revathy Auchère Francoise Norman Henrietta Markgren Per-Olof Gustavsson Susanne Schmidt Staffan Lundquist Stefan Forbes Louisa V Magon Nicholas J Paton Louise N Jameson Guy N L Eriksson Håkan Kettle Anthony J |
| Institution: | AstraZeneca R&D, S?dert?lje SE-151 85, Sweden. |
| Abstract: | Myeloperoxidase (MPO) is a prime candidate for promoting oxidative stress during inflammation. This abundant enzyme of neutrophils uses hydrogen peroxide to oxidize chloride to highly reactive and toxic chlorine bleach. We have identified 2-thioxanthines as potent mechanism-based inactivators of MPO. Mass spectrometry and x-ray crystal structures revealed that these inhibitors become covalently attached to the heme prosthetic groups of the enzyme. We propose a mechanism whereby 2-thioxanthines are oxidized, and their incipient free radicals react with the heme groups of the enzyme before they can exit the active site. 2-Thioxanthines inhibited MPO in plasma and decreased protein chlorination in a mouse model of peritonitis. They slowed but did not prevent neutrophils from killing bacteria and were poor inhibitors of thyroid peroxidase. Our study shows that MPO is susceptible to the free radicals it generates, and this Achilles' heel of the enzyme can be exploited to block oxidative stress during inflammation. |
| Keywords: | Enzyme Inactivation Inflammation Neutrophil Peroxidase Reactive Oxygen Species Hypochlorous Acid Myeloperoxidase |
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