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Hypoxia-inducible factor 1alpha stabilization by carbon monoxide results in cytoprotective preconditioning

The most salient feature of carbon monoxide (CO)-mediated cytoprotection is the suppression of inflammation and cell death. One of the important cellular targets of CO is the macrophage (mphi). Many studies have shown that exposure of mphi to CO results in the generation of an antiinflammatory pheno...

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Published in:	Proceedings of the National Academy of Sciences - PNAS 2007-03, Vol.104 (12), p.5109
Main Authors:	Chin, Beek Y, Jiang, Ge, Wegiel, Barbara, Wang, Hong J, Macdonald, Theresa, Zhang, Xu Chen, Gallo, David, Cszimadia, Eva, Bach, Fritz H, Lee, Patty J, Otterbein, Leo E
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Language:	English
Subjects:	Animals Apoptosis - drug effects Carbon Monoxide - pharmacology Cell Hypoxia - drug effects Cell Survival - drug effects Cytoprotection - drug effects Gene Expression Regulation - drug effects Humans Hypoxia-Inducible Factor 1, alpha Subunit - metabolism Interleukin-10 - metabolism Ischemic Preconditioning Lung - drug effects Lung - pathology Macrophages - cytology Macrophages - drug effects Mice Mitochondria - drug effects Oxygen - metabolism Reactive Oxygen Species - metabolism Reperfusion Injury - chemically induced RNA, Messenger - genetics RNA, Messenger - metabolism Thermodynamics Transforming Growth Factor beta - genetics Transforming Growth Factor beta - metabolism
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creator	Chin, Beek Y Jiang, Ge Wegiel, Barbara Wang, Hong J Macdonald, Theresa Zhang, Xu Chen Gallo, David Cszimadia, Eva Bach, Fritz H Lee, Patty J Otterbein, Leo E
description	The most salient feature of carbon monoxide (CO)-mediated cytoprotection is the suppression of inflammation and cell death. One of the important cellular targets of CO is the macrophage (mphi). Many studies have shown that exposure of mphi to CO results in the generation of an antiinflammatory phenotype; however, these reports have ignored the effect of CO alone on the cell before stimulation. Most investigations have focused on the actions of CO in modulating the response to noxious stimuli. We demonstrate here that exposure of mphi to CO results in a significant and transient burst of reactive oxygen species (ROS) arising from the mitochondria (mitochondria-deficient mphi do not respond to CO to produce ROS). The ROS promote rapid activation and stabilization of the transcription factor hypoxia-inducible factor 1alpha (HIF-1alpha), which regulates expression of genes involved in inflammation, metabolism, and cell survival. The increase in HIF-1alpha expression induced by CO results in regulated expression of TGF-beta, a potent antiinflammatory cytokine. CO-induced HIF-1alpha and TGF-beta expression are necessary to prevent anoxia/reoxygenation-induced apoptosis in mphi. Furthermore, blockade of HIF-1alpha using RNA interference and HIF-1alpha-cre-lox mphi resulted in a loss of TGF-beta expression and CO-induced protection. A similar mechanism of CO-induced protection was operational in vivo to protect against lung ischemia-reperfusion injury. Taken together, we conclude that CO conditions the mphi via a HIF-1alpha and TGF-beta-dependent mechanism and we elucidate the earliest events in mphi signaling that lead to and preserve cellular homeostasis at the site of injury.
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One of the important cellular targets of CO is the macrophage (mphi). Many studies have shown that exposure of mphi to CO results in the generation of an antiinflammatory phenotype; however, these reports have ignored the effect of CO alone on the cell before stimulation. Most investigations have focused on the actions of CO in modulating the response to noxious stimuli. We demonstrate here that exposure of mphi to CO results in a significant and transient burst of reactive oxygen species (ROS) arising from the mitochondria (mitochondria-deficient mphi do not respond to CO to produce ROS). The ROS promote rapid activation and stabilization of the transcription factor hypoxia-inducible factor 1alpha (HIF-1alpha), which regulates expression of genes involved in inflammation, metabolism, and cell survival. The increase in HIF-1alpha expression induced by CO results in regulated expression of TGF-beta, a potent antiinflammatory cytokine. CO-induced HIF-1alpha and TGF-beta expression are necessary to prevent anoxia/reoxygenation-induced apoptosis in mphi. Furthermore, blockade of HIF-1alpha using RNA interference and HIF-1alpha-cre-lox mphi resulted in a loss of TGF-beta expression and CO-induced protection. A similar mechanism of CO-induced protection was operational in vivo to protect against lung ischemia-reperfusion injury. 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subjects	Animals Apoptosis - drug effects Carbon Monoxide - pharmacology Cell Hypoxia - drug effects Cell Survival - drug effects Cytoprotection - drug effects Gene Expression Regulation - drug effects Humans Hypoxia-Inducible Factor 1, alpha Subunit - metabolism Interleukin-10 - metabolism Ischemic Preconditioning Lung - drug effects Lung - pathology Macrophages - cytology Macrophages - drug effects Mice Mitochondria - drug effects Oxygen - metabolism Reactive Oxygen Species - metabolism Reperfusion Injury - chemically induced RNA, Messenger - genetics RNA, Messenger - metabolism Thermodynamics Transforming Growth Factor beta - genetics Transforming Growth Factor beta - metabolism
title	Hypoxia-inducible factor 1alpha stabilization by carbon monoxide results in cytoprotective preconditioning
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