Original Article
Journal of Cerebral Blood Flow & Metabolism (2008) 28, 927–938; doi:10.1038/sj.jcbfm.9600582; published online 14 November 2007
Early release of HMGB-1 from neurons after the onset of brain ischemia
This work was supported by NIH R21NS056212-01A1, R01NS048198, and Massachusetts General Hospital Neuroscience Center Core Facility (NIH P30-NS045776). Jianhua Qiu was partly supported by AHA N0335154. John R Sims was supported by AHA 0535138N and NIH K08 NS049241. Sean I Savitz was supported by AHA 0475008N.
Jianhua Qiu1, Masaki Nishimura1, Yumei Wang1, John R Sims1, Sumei Qiu1, Sean I Savitz1, Salvatore Salomone1 and Michael A Moskowitz1
1Stroke and Neurovascular Regulation Laboratory, Department of Radiology, Massachusetts General Hospital, Charlestown, Massachusetts, USA
Correspondence: Dr J Qiu, Department of Radiology, Massachusetts General Hospital, 149, 13th Street, Room 6403, Charlestown, MA 02129, USA. E-mail: jqiu@partners.org
Received 2 July 2007; Revised 1 October 2007; Accepted 10 October 2007; Published online 14 November 2007.
Abstract
The nuclear protein high-mobility group box 1 (HMGB-1) promotes inflammation in sepsis, but little is known about its role in brain ischemia-induced inflammation. We report that HMGB-1 and its receptors, receptor for advanced glycation end products (RAGE), Toll-like receptor 2 (TLR2), and TLR4, were expressed in normal brain and in cultured neurons, endothelia, and glial cells. During middle cerebral artery occlusion (MCAO), in mice, HMGB-1 immunostaining rapidly disappeared from all cells within the striatal ischemic core from 1 h after onset of occlusion. High-mobility group box 1 translocation from nucleus to cytoplasm was observed within the cortical periinfarct regions 2 h after ischemic reperfusion (2 h MCAO). High-mobility group box 1 predominantly translocated to the cytoplasm or disappeared in cells that colabeled with the neuronal marker NeuN. Furthermore, RAGE was robustly expressed in the periinfarct region after MCAO. Cellular release of HMGB-1 was detected by immunoblotting of cerebrospinal fluid as early as 2 h after ischemic reperfusion (2 h MCAO). High-mobility group box 1 released from neurons, in vitro, after glutamate excitotoxicity, maintained biologic activity and induced glial expression of tumor necrosis factor 
(TNF). Anti-HMGB-1 antibody suppressed TNF upregulation in astrocytes exposed to conditioned media from glutamate-treated neurons. Moreover, TNF and the cytokine intercellular adhesion molecule-1 increased in cultured glia and endothelial cells, respectively, after adding recombinant HMGB-1. In conclusion, HMGB-1 is released early after ischemic injury from neurons and may contribute to the initial stages of the inflammatory response.
Keywords:
HMGB-1, NeuN, brain ischemia, MCAO, neuroinflammation
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