Abstract

Peripheral nerve is the only part of the nervous system that is commonly biopsied to evaluate human neurologic disease. Nerve biopsies should provide a valuable means of extending our understanding of the pathogenesis of neuropathies. To do so new, clinically appropriate methods of studying the specimens are required. This proposal will develop innovative means of examining human biopsies and apply these methods to specific questions.
Aim 1 will examine the participation of macrophages in a variety of neuropathies, using high resolution immunocytochemistry of teased nerve fibers and a panel of antibodies that will allow phenotyping the macrophage response.
Aim 1 will examine Schwann cells proliferation in such disorders as hypertrophic neuropathies due to Charcot-Marie-Tooth disease (HMSN I); these studies will utilize nuclear proliferation-associated monoclonal antibodies.
Aim 3 will examine Schwann cell expression of nerve growth factor receptor (NGF-R) in neuropathies; we anticipate that NGF-R will be found in a variety of demyelinating disorders as well as in axonal degenerations.
Aim 4 will examine the expression of growth-associated proteins in axons, asking to what extent to which they might provide an indication of early axonal disease.
Aim 5 will use in situ hybridization to examine the content of mRNAs for myelin proteins in Schwann cells in selected neuropathies. We anticipate that many of the approaches developed will find widespread application in the routine examination of peripheral nerve biopsies, and others will provide tools for use in research laboratories.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
5P01NS022849-09
Application #
3760756
Study Section
Project Start
Project End
Budget Start
Budget End
Support Year
9
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

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

  Publications

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
Xu, Z; Marszalek, J R; Lee, M K et al. (1996) Subunit composition of neurofilaments specifies axonal diameter. J Cell Biol 133:1061-9
Haney, C; Snipes, G J; Shooter, E M et al. (1996) Ultrastructural distribution of PMP22 in Charcot-Marie-Tooth disease type 1A. J Neuropathol Exp Neurol 55:290-9
Hsieh, S T; Choi, S; Lin, W M et al. (1996) Epidermal denervation and its effects on keratinocytes and Langerhans cells. J Neurocytol 25:513-24
Kidd, G; Andrews, S B; Trapp, B D (1996) Axons regulate the distribution of Schwann cell microtubules. J Neurosci 16:946-54
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
Trapp, B D; Kidd, G J; Hauer, P et al. (1995) Polarization of myelinating Schwann cell surface membranes: role of microtubules and the trans-Golgi network. J Neurosci 15:1797-807
Despres, P; Griffin, J W; Griffin, D E (1995) Effects of anti-E2 monoclonal antibody on sindbis virus replication in AT3 cells expressing bcl-2. J Virol 69:7006-14
Despres, P; Griffin, J W; Griffin, D E (1995) Antiviral activity of alpha interferon in Sindbis virus-infected cells is restored by anti-E2 monoclonal antibody treatment. J Virol 69:7345-8
McCarthy, B G; Hsieh, S T; Stocks, A et al. (1995) Cutaneous innervation in sensory neuropathies: evaluation by skin biopsy. Neurology 45:1848-55

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