Abstract

The purpose of the proposed research is to elucidate the rules which determine the response of immature CNS neurons to damage, the mechanisms which underlie the anatomical and functional reorganization that follows early CNS damage, and the factors which permit more successful reorganization i the neonate than in the adult CNS. We have demonstrated previously that embryonic neural tissue transplants modify the response of the immature spinal cord to damage by rescuing immature axotomized neurons from retrograde cell death and by supporting the growth of axons from the host CNS into the transplant. Spinal cord to spinal cord (homonymous) transplants support the persistent survival of axotomized neurons and elongation of their axons, whereas heteronymous (non-spinal cord) transplants only temporarily support this reorganization. Thus permanent reorganization resulting in recovery and/or sparing of function is a target-specific effect of the transplant. The current proposal is designed to identify cellular and molecular mechanisms underlying neuronal survival and axonal elongation after injury in the developing nervous system. We will determine the degree to which the capacity of immature CNS neurons for survival and axonal elongation after injury is regulated by factors intrinsic to the developing neuronal systems (for example the presence of axonal collaterals, ongoing synthesis of growth associated proteins) and the degree to which extrinsic environmental conditions (such as the presence of particular extracellular matrix components) regulate survival and growth and the degree to which intrinsic and extrinsic factors interact. Our model system (spinal cord injury at birth) allows us to study the effect of transplants on the development of undamaged axons in the corticospinal tract and on the survival of axotomized brainstem-spinal tract cells and subsequent re-growth of their axons. We will use quantitative methods to compare developing and regenerating neuronal populations to determine the extent to which their requirements for survival and axonal elongation differ and the extent to which they are similar. We will use neural tissue transplantation n vivo, neuroanatomical tracing (immunocytochemistry, horseradish peroxidase, and florescent tracers) at light and electron microscopic levels and in vitro tissue culture techniques to address these questions.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS019259-08
Application #
3399270
Study Section
Neurology B Subcommittee 2 (NEUB)
Project Start
1988-07-01
Project End
1994-06-30
Budget Start
1990-07-01
Budget End
1991-06-30
Support Year
8
Fiscal Year
1990
Total Cost
Indirect Cost

  Institution

Name
Georgetown University
Department
Type
Schools of Medicine
DUNS #
049515844
City
Washington
State
DC
Country
United States
Zip Code
20057

  Publications

Kim, Byung G; Dai, Hai-Ning; McAtee, Marietta et al. (2007) Labeling of dendritic spines with the carbocyanine dye DiI for confocal microscopic imaging in lightly fixed cortical slices. J Neurosci Methods 162:237-43
Ishii, Ken; Nakamura, Masaya; Dai, Haining et al. (2006) Neutralization of ciliary neurotrophic factor reduces astrocyte production from transplanted neural stem cells and promotes regeneration of corticospinal tract fibers in spinal cord injury. J Neurosci Res 84:1669-81
Nakamura, M; Okano, H; Toyama, Y et al. (2005) Transplantation of embryonic spinal cord-derived neurospheres support growth of supraspinal projections and functional recovery after spinal cord injury in the neonatal rat. J Neurosci Res 81:457-68
Nakamura, Masaya; Houghtling, Richard A; MacArthur, Linda et al. (2003) Differences in cytokine gene expression profile between acute and secondary injury in adult rat spinal cord. Exp Neurol 184:313-25
Bundesen, Liza Q; Scheel, Tracy Aber; Bregman, Barbara S et al. (2003) Ephrin-B2 and EphB2 regulation of astrocyte-meningeal fibroblast interactions in response to spinal cord lesions in adult rats. J Neurosci 23:7789-800
Bregman, Barbara S; Coumans, Jean-Valery; Dai, Hai Ning et al. (2002) Transplants and neurotrophic factors increase regeneration and recovery of function after spinal cord injury. Prog Brain Res 137:257-73
Qiu, Jin; Cai, Dongming; Dai, Haining et al. (2002) Spinal axon regeneration induced by elevation of cyclic AMP. Neuron 34:895-903
Cai, D; Qiu, J; Cao, Z et al. (2001) Neuronal cyclic AMP controls the developmental loss in ability of axons to regenerate. J Neurosci 21:4731-9
Coumans, J V; Lin, T T; Dai, H N et al. (2001) Axonal regeneration and functional recovery after complete spinal cord transection in rats by delayed treatment with transplants and neurotrophins. J Neurosci 21:9334-44
Nakamura, M; Bregman, B S (2001) Differences in neurotrophic factor gene expression profiles between neonate and adult rat spinal cord after injury. Exp Neurol 169:407-15

Showing the most recent 10 out of 35 publications