Abstract

We have discovered that Schwann cells, distal to an injury of sciatic nerve express high densities of nerve growth factor (NGF) receptors. We propose that Schwann cells, when deprived of axonal contact, both express NGF receptors and produce NGF. This results in an """"""""NGF-laden substratum"""""""" which provides tropic guidance and trophic support to facilitate regeneration of NGF responsive neurons. We propose to characterize the phenomenon of NGF receptor induction on Schwann cells after nerve injury, to assess the physiological significance of this phenomenon, and to determine the mechanism(s) involved in regulation of NGF receptors on Schwann cells. We shall describe by receptor quantitation and by microscopic localization the time course of receptor induction after transection or crush of sciatic nerve to determine effects of reinnervation and to provide a precise anatomical description of NGF receptor interactions during these processes. We shall determine whether a similar induction of NGF receptor occurs after various lesions within the CNS and whether NGF receptor induction only occurs on glial cells previously associated with axons of NGF responsive neurons. We have found that NGF receptors appear in high numbers when Schwann cells are cultured. We shall define the time course of receptor induction and the kinetic properties of the receptors. Once the culture system is well defined, it will be used to examine the mechanisms by which axonal interaction modulates NGF receptor density on Schwann cells. We shall examine the possibility that the NGF can directly exert effects on Schwann cells. In parallel with these experiments, NGF protein levels (two-site immunoassay) and NGF mRNA (quantitative Northern blot analysis) will be determined under similar conditions. Sites of NGF biosynthesis will be determined by in situ hybridization. We shall thus be able to correlate the phenomena and mechanisms controlling NGF receptor expression and NGF synthesis in cultured Schwann cells and in injured nerve. We shall test the hypothesis that the NGF- laden substratum is important in sympathetic axonal regeneration by assessing the effects of systemic or local NGF deprivation on regeneration after sciatic nerve crush. Lastly, we shall examine the possibility that, during development, Schwann cells bear NGF receptors by measuring NGF receptors in nerve during development and by localizing by EM immunohistochemistry NGF receptors in developing nerve. This project will provide an assessment of NGF receptors on Schwann cells and their possible role in Schwann cell/axon interactions.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS024679-04
Application #
3409482
Study Section
Neurology B Subcommittee 2 (NEUB)
Project Start
1987-04-01
Project End
1994-03-31
Budget Start
1990-04-01
Budget End
1991-03-31
Support Year
4
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Washington University
Department
Type
Schools of Medicine
DUNS #
062761671
City
Saint Louis
State
MO
Country
United States
Zip Code
63130

  Publications

Werth, J L; Deshmukh, M; Cocabo, J et al. (2000) Reversible physiological alterations in sympathetic neurons deprived of NGF but protected from apoptosis by caspase inhibition or Bax deletion. Exp Neurol 161:203-11
Franklin, J L; Johnson, E M (1998) Control of neuronal size homeostasis by trophic factor-mediated coupling of protein degradation to protein synthesis. J Cell Biol 142:1313-24
Easton, R M; Johnson, E M; Creedon, D J (1998) Analysis of events leading to neuronal death after infection with E1-deficient adenoviral vectors. Mol Cell Neurosci 11:334-47
Easton, R M; Deckwerth, T L; Parsadanian, A S et al. (1997) Analysis of the mechanism of loss of trophic factor dependence associated with neuronal maturation: a phenotype indistinguishable from Bax deletion. J Neurosci 17:9656-66
Miller, T M; Moulder, K L; Knudson, C M et al. (1997) Bax deletion further orders the cell death pathway in cerebellar granule cells and suggests a caspase-independent pathway to cell death. J Cell Biol 139:205-17
Creedon, D J; Johnson, E M; Lawrence, J C (1996) Mitogen-activated protein kinase-independent pathways mediate the effects of nerve growth factor and cAMP on neuronal survival. J Biol Chem 271:20713-8
Deckwerth, T L; Elliott, J L; Knudson, C M et al. (1996) BAX is required for neuronal death after trophic factor deprivation and during development. Neuron 17:401-11
Miller, T M; Johnson Jr, E M (1996) Metabolic and genetic analyses of apoptosis in potassium/serum-deprived rat cerebellar granule cells. J Neurosci 16:7487-95
Deshmukh, M; Vasilakos, J; Deckwerth, T L et al. (1996) Genetic and metabolic status of NGF-deprived sympathetic neurons saved by an inhibitor of ICE family proteases. J Cell Biol 135:1341-54
Bullock, E D; Johnson Jr, E M (1996) Nerve growth factor induces the expression of certain cytokine genes and bcl-2 in mast cells. Potential role in survival promotion. J Biol Chem 271:27500-8

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