Abstract

Wallerian degeneration, the process of axonal breakdown and clearance of axonal and myelln debris, follows focal transection of an axon from mechanical, thermal, or Ischemic causes. The pathologically similar process of distally predominant Wallerian-like degeneration characterizes many heritable metabolic, toxic and Inflammatory disorders of nerve. Teleologically, Wallerian degeneration serves the purpose of clearing the distal stump and preparing the way for regeneration. The pivotal event Initiating most of the sequence of Wallerlan degeneration Is the breakdown of the axon and an early event in axonal breakdown is granular disintegration of the axonal cytoskeleton (GDC). Previous reports and our preliminary data suggest that GDC Is the consequence of limited cleavage of neurofilaments and other cytoskeletal proteins by the ion-sensitive protease calpain. We have shown that axonal survival can be markedly prolonged by preventing entry of extracellular calcium and by cellpermeant calpain blockers. The goals of this project are to understand the mechanism of axonal degeneration as Initiated by transection of nerve fibers, to develop methods for preventing or retarding axonal degeneration, and to manipulate the production of factors that promote nerve regeneration, such as nerve growth factor (NGF) so that retarding axonal degeneration need not prevent axonal regeneration. To accomplish these goals we will complete a definitive analysis of the spatiotemporal sequence of Wallerian degeneration use short term organ cultures of mature nerve segments in vitro to dissect the mechanisms of GDC, and apply these results to means of retarding Wallerian degeneration in vivo. Finally we will use combined immunocytochemistry and in situ hybridization to examine the phenotypic changes and neurotrophin production of target cells in the skin. In this system we will determine whether nerve growth factor production can be dissociated from axonal breakdown. The results will provide new insights into a fundamental and prevalent pathologic process in nervous system disease, and they should identify ways of protecting nerve fibers and of maintaining function in monophasic inflammatory or toxic disorders of nerve.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS014784-18
Application #
2262688
Study Section
Neurological Sciences Subcommittee 1 (NLS)
Project Start
1978-07-01
Project End
1999-06-30
Budget Start
1995-07-01
Budget End
1996-06-30
Support Year
18
Fiscal Year
1995
Total Cost
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Neurology
Type
Schools of Medicine
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Hoke, Ahmet; Ho, Tony; Crawford, Thomas O et al. (2003) Glial cell line-derived neurotrophic factor alters axon schwann cell units and promotes myelination in unmyelinated nerve fibers. J Neurosci 23:561-7
Tsao, J W; George, E B; Griffin, J W (1999) Temperature modulation reveals three distinct stages of Wallerian degeneration. J Neurosci 19:4718-26
McArthur, J C; Stocks, E A; Hauer, P et al. (1998) Epidermal nerve fiber density: normative reference range and diagnostic efficiency. Arch Neurol 55:1513-20
Hoffman, P N; Luduena, R F (1996) The axonal transport of beta III-tubulin is altered in both branches of sensory axons after injury of the rat sciatic nerve. Brain Res 708:182-4
Hoffman, P N; Luduena, R F (1996) Changes in the isotype composition of beta-tubulin delivered to regenerating sensory axons by slow axonal transport. Brain Res 742:329-33
Glass, J D; Schryer, B L; Griffin, J W (1994) Calcium-mediated degeneration of the axonal cytoskeleton in the Ola mouse. J Neurochem 62:2472-5
Archer, D R; Watson, D F; Griffin, J W (1994) Phosphorylation-dependent immunoreactivity of neurofilaments and the rate of slow axonal transport in the central and peripheral axons of the rat dorsal root ganglion. J Neurochem 62:1119-25
Hoffman, P N; Lopata, M A; Watson, D F et al. (1992) Axonal transport of class II and III beta-tubulin: evidence that the slow component wave represents the movement of only a small fraction of the tubulin in mature motor axons. J Cell Biol 119:595-604
Watson, D F; Fittro, K P; Hoffman, P N et al. (1991) Phosphorylation-related immunoreactivity and the rate of transport of neurofilaments in chronic 2,5-hexanedione intoxication. Brain Res 539:103-9
Griffin, J W; Clark, A C; Parhad, I et al. (1991) The neuronal cytoskeleton in disorders of the motor neuron. Adv Neurol 56:103-13

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