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Inflammatory reaction after focal cerebral ischemia in mouse
作者姓名:Wang ZQ  Chen XC  Yang GY  Zhou LF
作者单位:Department of Neurosurgery,Department of Neurosurgery,Center for Cerebrovascular Research,Department of Neurosurgery Huashan Hospital,Fudan University,Shanghai 200040,China,Huashan Hospital,Fudan University,Shanghai 200040,China,San Francisco,General Hospital University of California in San Francisco,94110,USA,Huashan Hospital,Fudan University,Shanghai 200040,China
摘    要:Inflammationisacriticalprocessafterstroke 1 Studieshaverevealedtheover expressionofinflammatoryfactorsandtheaccumulationofinflammatorycellsinischemictissues 1,2  Intercellularadhesionmolecule 1(ICAM 1) ,oneoftheadhesionmolecules ,isexpressedconstitutivelyonthesurfaceoftheendotheliumandcanbeupregulatedbyharmfulstimulation 1,2  ReportsalsoshowedthatinflammatoryfactorsincludingMCP 1,IL 1βandTNFαcaninducetheoverexpressionofICAM 1 3 7CD11b/CD18(Mac 1) ,asubgroupoftheintegrinfamilyofadh…

关 键 词:大脑中动脉缺血  炎症反应  动物模型  细胞粘附分子  病理机制

Inflammatory reaction after focal cerebral ischemia in mouse
Wang ZQ,Chen XC,Yang GY,Zhou LF.Inflammatory reaction after focal cerebral ischemia in mouse[J].Chinese Medical Journal,2004,117(4):586-591.
Authors:Wang Zhi-Qiu  Chen Xian-Cheng  Yang Guo-Yuan  Zhou Liang-Fu
Institution:1. Department of Neurosurgery, Huashan Hospital, Fudan University, Shanghai 200040, China
2. Center for Cerebrovascular Research, San Francisco, General Hospital University of California in San Francisco, 94110, USA
Abstract:Background In response to the inflammatory reaction, circulating leukocytes aggregate and adhere to the endothelial cells and eventually pervade into tissues, resulting in cell damage. This study was to detect the inflammatory reactions in mouse focal cerebral ischemia and their distinct characteristics in the ischemic basal ganglia and surrounding cortex.Methods Mice were subjected to permanent occlusion of the left middle cerebral artery (MCAO) by introducing a suture for 2 to 120 hours. The expression of intercellular adhesion molecule 1 (ICAM-1) and Mac-1 was determined immunohistochemically. The myeloperoxidase (MPO) activity of the ischemic regions was measured.Results Four hours after MCAO, the number of ICAM-1 positive vessels in the ischemic basal ganglia increased (9.2±2.8 per mm2), peaked at 48 hours (29.6±4.8 per mm2), and decreased after 72 hours. In the ischemic cortex, the number increased rapidly 4 hours after MCAO (19.4±6.1 per mm2), peaked at 48 hours (44.4±16.8 per mm2), and declined after 72 hours. Mac-1 positive cells were seen in the ischemic basal ganglia (3.4±1.2 per mm2) 12 hours after MCAO, peaked after 48 hours (20.2±6.3 per mm2), and decreased after 72 hours. In the ischemic cortex, however, the number increased 4 hours after MCAO (4.3±1.7 per mm2), peaked after 48 hours (20.9±8.4 per mm2), and remained high at 120 hours. The MPO activity increased in the ischemic basal ganglia 12 hours after MCAO (0.111±0.023 U/g), peaked after 24 hours (0.194±0.059 U/g), and decreased after 72 hours. In the ischemic cortex, the MPO activity increased 12 hours after MCAO (0.110±0.032 U/g), peaked after 24 hours (0.210±0.067 U/g), and remained elevated at 120 hours.Conclusions The increased expression of ICAM-1 in the ischemic brain of mouse in the early phase of MCAO followed by the over-expression of Mac-1 and the increased MPO activity suggests that focal ischemia leads to early onset of inflammation. The inflammatory response is more persistent and intensive in the ischemic cortex than in the ischemic basal ganglia.
Keywords:cerebral ischemia  regional blood flow  inflammation  endothelium cell adhesion molecules  leukocytes  myeloperoxidase  mice
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