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Single low-dose lipopolysaccharide preconditioning:neuroprotective against axonal injury and modulates glial cells 被引量:1
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作者 Ryan C.Turner Zachary J.Naser +5 位作者 brandon p.lucke-wold Aric F.Logsdon Reyna L.Vangilder Rae R.Matsumoto Jason D.Huber Charles L.Rosen 《Neuroimmunology and Neuroinflammation》 2017年第1期6-15,共10页
Aim:Over 7 million traumatic brain injuries (TBI) are reported each year in the United States.However,treatments and neuroprotection following TBI are limited because secondary injury cascades are poorly understood.Li... Aim:Over 7 million traumatic brain injuries (TBI) are reported each year in the United States.However,treatments and neuroprotection following TBI are limited because secondary injury cascades are poorly understood.Lipopolysaccharide (LPS) administration before controlled cortical impact can contribute to neuroprotection.However,the underlying mechanisms and whether LPS preconditioning confers neuroprotection against closed-head injuries remains unclear.Methods:The authors hypothesized that preconditioning with a low dose of LPS (0.2 mg/kg) would regulate glial reactivity and protect against diffuse axonal injury induced by weight drop.LPS was administered 7 days prior to TBI.LPS administration reduced locomotion,which recovered completely by time of injury.Results:LPS preconditioning significantly reduced the post-injury gliosis response near the corpus callosum,possibly by downregulating the oncostatin M receptor.These novel findings demonstrate a protective role of LPS preconditioning against diffuse axonal injury.LPS preconditioning successfully prevented neurodegeneration near the corpus callosum,as measured by fluorojade B.Conclusion:Further work is required to elucidate whether LPS preconditioning confers long-term protection against behavioral deficits and to elucidate the biochemical mechanisms responsible for LPS-induced neuroprotective effects. 展开更多
关键词 LIPOPOLYSACCHARIDE PRECONDITIONING oncostatin M receptor diffuse axonal injury GLIOSIS NEUROPROTECTION
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