Abstract

This proposal explores expression of the rapidly inducible c-fos and heat shock genes following neural injury. Molecular mechanisms of injury are poorly understood and new indicators of injury are needed since many animal studies use histological stains to assess the efficacy of therapeutic drug regimens for ameliorating the CNS damage caused by stroke, excitotoxins, and head injury. Many histological stains have serious limitations including problems detecting early injury, particularly to single cells. Fos, the gene product of c-fos, is rapidly induced in the nuclei of single cells throughout cortex and amygdala following focal cortical lesions and focal cortical injections of NGF. Experiments will test the hypothesis that local release of NGF and other molecules at the sites of injury activate cholinergic neurons in the nucleus Basalis of Meynert (NBM) which in turn project upon and induce Fos in cells throughout cortex. We will determine (a) which cells express Fos and (b) which trophic substances, when injected into cortex or into NBM, induce Fos, detected immunocytochemically, and c-fos mRNA, detected using Northern blots and in situ hybridization. Heat shock proteins (HSPs) are also rapidly expressed following injury. Stroke, diffuse forebrain ischemia, systemic and local injections of kainic acid, and local injections of kynurenic acid and MK801 rapidly induce the heart shock protein, HSP72, in single neurons and glia. The time course and topographic distribution of HSP72 induction following ischemic injury will be described. This will be correlated with the regions where cell death or cell survival occurs on standard histological stains. The induction of HSP72 produced by excitatory amino acid agonists and antagonists will be studied in primary cultures of neurons and glia. Moreover, experiments will test whether induction of HSP72 proteins protects cultured neurons and glia from otherwise lethal injuries. Future studies will determine whether prior induction of either the heat shock or c-fos genes protects the brain from injury.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS028167-02
Application #
3414646
Study Section
Neurology B Subcommittee 2 (NEUB)
Project Start
1990-06-01
Project End
1993-05-31
Budget Start
1991-06-01
Budget End
1992-05-31
Support Year
2
Fiscal Year
1991
Total Cost
Indirect Cost

  Institution

Name
University of California San Francisco
Department
Type
Schools of Medicine
DUNS #
073133571
City
San Francisco
State
CA
Country
United States
Zip Code
94143

  Publications

Xu, Huichun; Lu, Aigang; Sharp, Frank R (2011) Regional genome transcriptional response of adult mouse brain to hypoxia. BMC Genomics 12:499
Zhan, Xinhua; Ander, Bradley P; Jickling, Glen et al. (2010) Brief focal cerebral ischemia that simulates transient ischemic attacks in humans regulates gene expression in rat peripheral blood. J Cereb Blood Flow Metab 30:110-8
Jickling, Glen C; Zhan, Xinhua; Ander, Bradley P et al. (2010) Genome response to tissue plasminogen activator in experimental ischemic stroke. BMC Genomics 11:254
Lu, Aigang; Clark, Joseph F; Ran, Ruiqiong et al. (2009) Down-regulation of interleukin 7 mRNA by hypoxia is calcium dependent. Neurol Res 31:545-9
Lu, Aigang; Clark, Joseph F; Broderick, Joseph P et al. (2009) Mechanical reperfusion is associated with post-ischemic hemorrhage in rat brain. Exp Neurol 216:407-12
Lu, Aigang; Clark, Joseph F; Broderick, Joseph P et al. (2008) Reperfusion activates metalloproteinases that contribute to neurovascular injury. Exp Neurol 210:549-59
Zhan, Xinhua; Kim, Charles; Sharp, Frank R (2008) Very brief focal ischemia simulating transient ischemic attacks (TIAs) can injure brain and induce Hsp70 protein. Brain Res 1234:183-97
Xu, Huichun; Tang, Yang; Liu, Da-Zhi et al. (2008) Gene expression in peripheral blood differs after cardioembolic compared with large-vessel atherosclerotic stroke: biomarkers for the etiology of ischemic stroke. J Cereb Blood Flow Metab 28:1320-8
Liu, Da-Zhi; Cheng, Xi-Yuan; Ander, Bradley P et al. (2008) Src kinase inhibition decreases thrombin-induced injury and cell cycle re-entry in striatal neurons. Neurobiol Dis 30:201-11
Gregg, Jeffrey P; Lit, Lisa; Baron, Colin A et al. (2008) Gene expression changes in children with autism. Genomics 91:22-9

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