Endogenous adult neurogenesis and cognitive function recovery following traumatic brain injury in the rat hippocampus

BACKGROUND:Endogenous neural progenitor cells play a beneficial role for cognitive recovery following traumatic brain injury.However,there are few classification-control studies aimed at varying graded brain trauma.OBJECTIVE:To observe the effects of adult endogenous neurogenesis on cognitive functi...

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Published inNeural regeneration research Vol. 5; no. 9; pp. 645 - 650
Main Author Wangmiao Zhao Linchun Huan Yan Zhao Jie Zhao Qi Zhang Lin Zhang Rong Yan Shuyuan Yang Xinyu Yang
Format Journal Article
LanguageEnglish
Published Department of Neurosurgery,Tianjin Medical University General Hospital,Tianjin Neurology Institute,Tianjin Key Laboratory of Injuries,Variations and Regeneration of Nervous System,Tianjin 300052,China%Department of Neurosurgery,Tianjin Medical University General Hospital,Tianjin Neurology Institute,Tianjin Key Laboratory of Injuries,Variations and Regeneration of Nervous System,Tianjin 300052,China 15.05.2010
Tianjin People's Hospital,Tianjin 300121,China
Department of Neurosurgery,General Hospital of Chinese PLA,Beijing 100853,China%Department of Neurosurgery,Tianjin Medical University General Hospital,Tianjin Neurology Institute,Tianjin Key Laboratory of Injuries,Variations and Regeneration of Nervous System,Tianjin 300052,China
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Summary:BACKGROUND:Endogenous neural progenitor cells play a beneficial role for cognitive recovery following traumatic brain injury.However,there are few classification-control studies aimed at varying graded brain trauma.OBJECTIVE:To observe the effects of adult endogenous neurogenesis on cognitive function repair and regeneration of neural progenitor cells following varying graded traumatic hippocampal injury to determine the significance of endogenous neurogenesis in the repair of brain injury.DESIGN,TIME AND SETTING:A randomized,controlled,animal experiment was performed at the Key Laboratory of Injuries,Variations and Regeneration of Nervous System,Tianjin Medical University General Hospital,from February to October 2009.MATERIALS:Mouse anti-rat 5-bromodeoxyuridine (BrdU) and neuronal nuclei (NeuN) monoclonal antibodies were purchased from Millipore Corporation,USA.METHODS:A total of 45 Wistar rats were randomly assigned to three groups.Mild and severe injury groups were respectively subjected to (182 ± 2) kPa and (284 ± 4) kPa lateral fluid percussion to establish models of brain injury,and the control group was subjected to surgery with no lateral fluid percussion.MAIN OUTCOME MEASURES:Cognitive function was estimated using the Morris water maze.Proliferation,survival,and differentiation of newly generated cells in the injured hippocampus were observed through the use of immunofluorescent staining.RESULTS:At 7 days post-injury,the number of BrdU+ cells in the hippocampal dentate gyrus significantly increased in the mild and severe injury groups compared with the control group (P〈0.01).At 61 days post-injury,the number of BrdU7NeuN+ cells in the hippocampal dentate gyrus was significantly greater in the mild injury group compared with the severe injury and control groups (P〈 0.01).In addition,the control group exhibited the greatest proportion of surviving cells that differentiated into mature neurons compared with the injury groups (P〈 0.01).Moreover,at 61 days post-injury,cognitive function in rats with mild injury recovered to normal levels,whereas the severe injury group exhibited cognitive deficits (P〈 0.01).CONCLUSION:Traumatic brain injury may be a stimulation factor for proliferation of neural progenitor cells in the adult hippocampus but severe brain trauma does not lead to an increased number of newly generated cells.Endogenous adult neurogenesis repairs neurological functions to an extent.However,recovery of neurological function remains limited following severe traumatic brain injury.
Bibliography:cognitive function
brain injury
R
Morris water maze
neural regeneration
traumatic brain injury;hippocampus;Morris water maze;neurogenesis;cognitive function;brain injury;neural regeneration
hippocampus
traumatic brain injury
neurogenesis
11-5422/R
ISSN:1673-5374
DOI:10.3969/j.issn.1673-5374.2010.09.001