Abstract

This project seeks to identify the cellular mechanisms that regulate neurite outgrowth and synapse replacement in the hippocampus in response to injury and the effect of aging on these processes. Studies conducted during the previous funding period argue against the notion that reactive synaptogenesis involves a unitary set of cellular responses common to all neurons in the brain but more likely involves specific sets of partially overlapping developmental signals that are cell type, brain region and lesion specific. In addition, while it was once believed that degenerative disease of the brain can be represented by simple cell loss that leads to functional decline, it is now known that the injured brain represents a composite of various adaptive responses which work to preserve and repair the brain's synaptic circuits against a background of ongoing cell death. However, while previous anatomical studies have readily demonstrated the ability of neurons to adapt and form new synaptic circuits in response to brain injury the cellular and molecular mechanisms that regulate reactive synaptogenesis and the effect of aging on these processes remain unclear. The studies proposed are a direct extension of the work completed previously and will test three working hypotheses: 1) that the observed delayed but enhanced sprouting response of commissural/associational axons following a combined lesion of the entorhinal cortex/fimbria fornix (EC/FF) is selective for the loss of cholinergic input from the septum/diagonal band and input from the entorhinal cortex; 2) that in response to injury different sets of growth associated proteins and trophic factors regulate neurite outgrowth in projection neurons that terminate in different laminae of the dentate gyrus (DG); and 3) that the new pattern of synaptic innervation that is formed in the DG following the EC/FF lesion results in the formation of a pattern of aberrant neural circuits which increases the vulnerability of target neurons to injury, inhibits information processing and thus, limits the chance of functional recovery. The investigators will use experimental deafferentation lesions in rats to model different combinations of neurotransmitter deficits that may affect neurite outgrowth and synapse replacement in the DG following brain injury. In addition, they will screen aged rats prior to surgery, using the Morris water maze, to identify subsets of old rats with hippocampal deficits that may alter their ability to respond to the lesion. They will also assess the rate of functional recovery at various times postlesion to correlate with their morphological and molecular data. Morphological remodeling of afferent input to the DG will be evaluated using light microscopic histochemical and ultrastructural methods; while the synaptic physiology of the anatomically reorganized hippocampus will be examined by electrophysiological analysis. In addition, they will use in situ hybridization and western blot methods to define the time course of changes in the levels of mRNAs and proteins that they hypothesize are associated with the promotion of neurite outgrowth and synapse replacement in the hippocampus (i.e. GAP-43, SCG-10, BDNF, trkB and SNAP-25).

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS030426-08
Application #
6126241
Study Section
Neurology B Subcommittee 2 (NEUB)
Program Officer
Sheehy, Paul A
Project Start
1991-09-30
Project End
2001-11-30
Budget Start
1999-12-01
Budget End
2001-11-30
Support Year
8
Fiscal Year
2000
Total Cost
$216,779
Indirect Cost

  Institution

Name
University of Southern California
Department
Type
Organized Research Units
DUNS #
072933393
City
Los Angeles
State
CA
Country
United States
Zip Code
90089

  Publications

Snyder, S E; Cheng, H W; Murray, K D et al. (1998) The messenger RNA encoding VGF, a neuronal peptide precursor, is rapidly regulated in the rat central nervous system by neuronal activity, seizure and lesion. Neuroscience 82:7-19
Schauwecker, P E; McNeill, T H (1996) Dendritic remodeling of dentate granule cells following a combined entorhinal cortex/fimbria fornix lesion. Exp Neurol 141:145-53
Snyder, S E; Li, J; Schauwecker, P E et al. (1996) Comparison of RPTP zeta/beta, phosphacan, and trkB mRNA expression in the developing and adult rat nervous system and induction of RPTP zeta/beta and phosphacan mRNA following brain injury. Brain Res Mol Brain Res 40:79-96
Kohama, S G; Goss, J R; Finch, C E et al. (1995) Increases of glial fibrillary acidic protein in the aging female mouse brain. Neurobiol Aging 16:59-67
Schauwecker, P E; Cheng, H W; Serquinia, R M et al. (1995) Lesion-induced sprouting of commissural/associational axons and induction of GAP-43 mRNA in hilar and CA3 pyramidal neurons in the hippocampus are diminished in aged rats. J Neurosci 15:2462-70
Schauwecker, P E; McNeill, T H (1995) Enhanced but delayed axonal sprouting of the commissural/associational pathway following a combined entorhinal cortex/fimbria fornix lesion. J Comp Neurol 351:453-64
Day, J R; Laping, N J; Lampert-Etchells, M et al. (1993) Gonadal steroids regulate the expression of glial fibrillary acidic protein in the adult male rat hippocampus. Neuroscience 55:435-43
Beck, K D; Lamballe, F; Klein, R et al. (1993) Induction of noncatalytic TrkB neurotrophin receptors during axonal sprouting in the adult hippocampus. J Neurosci 13:4001-14