Abstract

This application is for the continuation of a research program on the recovery of function after neural damage. The proposed experiments will be performed on the peripheral nervous system due to its relative anatomical and biochemical simplicity and to its accessibility; however, we expect many of our findings to be applicable to the central nervous system as well. Biochemical changes in the cell bodies of peripheral neurons are thought to be related to survival and regeneration of the damaged neurons. In the present proposal, we focus on increases in the expression of certain neuropeptides in peripheral neurons after axotomy, with particular emphasis on sympathetic neurons in the rat superior cervical ganglion (SCG). Recent evidence suggests that some of these neuropeptides may act as trophic agents in the nervous system. A combination of biochemical and histochemical techniques, including radioimmunoassay, Northern blot analysis, immunohistochemistry and in situ hybridization, will be used to measure specific neuropeptides and their associated mRNA's.
The specific aims of the proposal are l)to determine the neuropeptide phenotype (s) of neurons in the SCG after axotomy by assaying immunoreactivity for ten peptides selected based on strict criteria, 2)to compare this phenotype to the neuropeptide phenotypes of axotomized sensory and motor neurons, 3)to examine whether changes in the level of peptides in the SCG are accompanied by changes in their mRNA's, 4)to investigate whether similar changes in peptide expression in sympathetic neurons are elicited by other manipulations that interfere with communication between sympathetic neurons and their target tissues and to determine 5)the involvement of specific differentiation factors and 6)non-neuronal cells in these changes in expression. The long term objective of this research is to understand the molecular and cellular mechanisms that promote or inhibit functional recovery after neural damage, such as that caused by stroke, trauma, and degenerative neurological disease. In addition, the results will be relevant to more general issues of the regulation of gene expression in the nervous system.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS017512-12
Application #
2263220
Study Section
Neurology B Subcommittee 2 (NEUB)
Project Start
1981-07-01
Project End
1997-12-31
Budget Start
1995-01-01
Budget End
1995-12-31
Support Year
12
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Case Western Reserve University
Department
Neurosciences
Type
Schools of Medicine
DUNS #
077758407
City
Cleveland
State
OH
Country
United States
Zip Code
44106

  Publications

Niemi, Jon P; Filous, Angela R; DeFrancesco, Alicia et al. (2017) Injury-induced gp130 cytokine signaling in peripheral ganglia is reduced in diabetes mellitus. Exp Neurol 296:1-15
Lingappa, Jaisri R; Zigmond, Richard E (2013) Limited recovery of pineal function after regeneration of preganglionic sympathetic axons: evidence for loss of ganglionic synaptic specificity. J Neurosci 33:4867-74
Niemi, Jon P; DeFrancesco-Lisowitz, Alicia; Roldán-Hernández, Lilinete et al. (2013) A critical role for macrophages near axotomized neuronal cell bodies in stimulating nerve regeneration. J Neurosci 33:16236-48
Zigmond, Richard E (2012) Cytokines that promote nerve regeneration. Exp Neurol 238:101-6
Pellegrino, Michael J; Parrish, Diana C; Zigmond, Richard E et al. (2011) Cytokines inhibit norepinephrine transporter expression by decreasing Hand2. Mol Cell Neurosci 46:671-80
Hyatt Sachs, H; Rohrer, H; Zigmond, R E (2010) The conditioning lesion effect on sympathetic neurite outgrowth is dependent on gp130 cytokines. Exp Neurol 223:516-22
Habecker, Beth A; Sachs, Hilary Hyatt; Rohrer, Hermann et al. (2009) The dependence on gp130 cytokines of axotomy induced neuropeptide expression in adult sympathetic neurons. Dev Neurobiol 69:392-400
Sachs, Hilary H; Wynick, David; Zigmond, Richard E (2007) Galanin plays a role in the conditioning lesion effect in sensory neurons. Neuroreport 18:1729-33
Hyatt Sachs, H; Schreiber, R C; Shoemaker, S E et al. (2007) Activating transcription factor 3 induction in sympathetic neurons after axotomy: response to decreased neurotrophin availability. Neuroscience 150:887-97
Zigmond, Richard E; Vaccariello, Stacey A (2007) Activating transcription factor 3 immunoreactivity identifies small populations of axotomized neurons in rat cervical sympathetic ganglia after transection of the preganglionic cervical sympathetic trunk. Brain Res 1159:119-23

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