Abstract

Surgical repair of injured peripheral nerve often fails to restore adequate function. Misdriction of regenerating axons is a primary cause of this failure. Motor axons reaching skin provide no function and block the pathways which they occupy; cutaneous axons reaching muscle may function, but will provide incorrect information. Recent experiments suggest a possible solution to this problem. Motor axons regenerating in the rat femoral nerve produce multiple collaterals sprouts; motor/sensory specificity is improved by pruning collaterals from cutaneous nerve while keeping those in muscle nerve. Specificity may be enhanced by crushing the nerve before repair to increase collateral sprout formation and pathway sampling. If a similar effect could be produced at the time of nerve suture, the outcome of clinical nerve repair could be substantially improved. The proposed experiments are designed to further characterize the process of specificity generation through collateral pruning, and to identify techniques for its amplification which could be applied to clinical nerve repair.
Aim I more clearly defines the mechanism by which nerve crush increases specificity, and seeks to correlate increased specificity with improved function.
Aim II seeks to stimulate regenerative collateral sprouting of motor axons and subsequent regeneration specificityby application of trophic factors directly the repair site in a controlled manner. The function resulting from these manipulations will be correlated with regeneration specificity. These experiments open the way to direct clinical application of specificity enhancement.
Aim III takes advantage of the greater specificity observed in juveniles to gain further insights into the mechanism of motor/sensory specificity, and introduces a novel nerve graft model which confornts adult pathways with juvenile axons and vice versa, to identify components which deteriorate with age. The extent of collateral sprouting in juvenile and aged rats will be correlated with final regeneration specificity.
Aim I V Evidence for pruning of motor axon collaterals from cutaneous nerve has been obtained with axon tracing techniques. These experiments will seek morphologic and electrophysiologic confirmation of pruning.
Aim V extends our observations of specific motor pathway characteristics to compare motor and sensory nerve as graft for regenerating motor axons. Preliminary experiments suggest that motor nerve is in fact superior, a finding which if confirmed will have immediate, direct clinical relevance.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
3R01NS034484-02S2
Application #
6339902
Study Section
Special Emphasis Panel (ZRG1 (01))
Program Officer
Chiu, Arlene Y
Project Start
1997-04-01
Project End
2000-03-31
Budget Start
1998-04-01
Budget End
2000-03-31
Support Year
2
Fiscal Year
2000
Total Cost
$12,553
Indirect Cost

  Institution

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

  Publications

O'Daly, Andres; Rohde, Charles; Brushart, Thomas (2016) The topographic specificity of muscle reinnervation predicts function. Eur J Neurosci 43:443-50
Wright, Megan C; Mi, Ruifa; Connor, Emmalynn et al. (2014) Novel roles for osteopontin and clusterin in peripheral motor and sensory axon regeneration. J Neurosci 34:1689-700
Siddique, Rezina; Vyas, Alka; Thakor, Nitish et al. (2014) A two-compartment organotypic model of mammalian peripheral nerve repair. J Neurosci Methods 232:84-92
Abdullah, M; O'Daly, A; Vyas, A et al. (2013) Adult motor axons preferentially reinnervate predegenerated muscle nerve. Exp Neurol 249:1-7
Brushart, T M; Aspalter, M; Griffin, J W et al. (2013) Schwann cell phenotype is regulated by axon modality and central-peripheral location, and persists in vitro. Exp Neurol 247:272-81
Udina, E; Ladak, A; Furey, M et al. (2010) Rolipram-induced elevation of cAMP or chondroitinase ABC breakdown of inhibitory proteoglycans in the extracellular matrix promotes peripheral nerve regeneration. Exp Neurol 223:143-52
Höke, Ahmet; Brushart, Thomas (2010) Introduction to special issue: Challenges and opportunities for regeneration in the peripheral nervous system. Exp Neurol 223:1-4
Vyas, Alka; Li, Zhaobo; Aspalter, Manuela et al. (2010) An in vitro model of adult mammalian nerve repair. Exp Neurol 223:112-8
Aspalter, Manuela; Vyas, Alka; Feiner, Jeffrey et al. (2009) Modification of Schwann cell gene expression by electroporation in vivo. J Neurosci Methods 176:96-103
Geremia, Nicole M; Gordon, Tessa; Brushart, Thomas M et al. (2007) Electrical stimulation promotes sensory neuron regeneration and growth-associated gene expression. Exp Neurol 205:347-59

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