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Publication : Carbon monoxide induced PPARĪ³ SUMOylation and UCP2 block inflammatory gene expression in macrophages.

First Author  Haschemi A Year  2011
Journal  PLoS One Volume  6
Issue  10 Pages  e26376
PubMed ID  22046279 Mgi Jnum  J:179711
Mgi Id  MGI:5302920 Doi  10.1371/journal.pone.0026376
Citation  Haschemi A, et al. (2011) Carbon monoxide induced PPARgamma SUMOylation and UCP2 block inflammatory gene expression in macrophages. PLoS One 6(10):e26376
abstractText  Carbon monoxide (CO) dampens pro-inflammatory responses in a peroxisome proliferator-activated receptor-gamma (PPARgamma) and p38 mitogen-activated protein kinase (MAPK) dependent manner. Previously, we demonstrated that CO inhibits lipopolysaccharide (LPS)-induced expression of the proinflammatory early growth response-1 (Egr-1) transcription factor in macrophages via activation of PPARgamma. Here, we further characterize the molecular mechanisms by which CO modulates the activity of PPARgamma and Egr-1 repression. We demonstrate that CO enhances SUMOylation of PPARgamma which we find was attributed to mitochondrial ROS generation. Ectopic expression of a SUMOylation-defective PPARgamma-K365R mutant partially abolished CO-mediated suppression of LPS-induced Egr-1 promoter activity. Expression of a PPARgamma-K77R mutant did not impair the effect of CO. In addition to PPARgamma SUMOylation, CO-activated p38 MAPK was responsible for Egr-1 repression. Blocking both CO-induced PPARgamma SUMOylation and p38 activation, completely reversed the effects of CO on inflammatory gene expression. In primary macrophages isolated form C57/BL6 male mice, we identify mitochondrial ROS formation by CO as the upstream trigger for the observed effects on Egr-1 in part through uncoupling protein 2 (UCP2). Macrophages derived from bone marrow isolated from Ucp2 gene Knock-Out C57/BL6 mice (Ucp2(-/-)), produced significantly less ROS with CO exposure versus wild-type macrophages. Moreover, absence of UCP2 resulted in a complete loss of CO mediated Egr-1 repression. Collectively, these results indentify p38 activation, PPARgamma-SUMOylation and ROS formation via UCP2 as a cooperative system by which CO impacts the inflammatory response.
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