Abstract

Spinal cord injury frequently results in permanent disruption of sensory and motor pathways and irreversible functional loss due to the inability of axons in the central nervous system to regenerate. Studies of spinal injury reported during the last decade suggest that inhibitory signals in injured spinal cord tissue contribute to regeneration failure. The identities of these inhibitory signals are largely unknown. Efforts to understand axon guidance during development have led to the identification of many axon-repellent molecules. These proteins belong to a small number of gene families. One such gene family is the semaphorins. Recently published studies suggest semaphorins may play a role in adult animals as well. These demonstrated that the expression of Semaphorin3A, a type 3 secreted semaphorin, is up-regulated in response to central nervous system injury. In addition, adult sensory neurons are repelled by secreted semaphorins. The goal of this application is to begin testing the hypothesis that secreted semaphorins contribute to regeneration failure after spinal cord injury. In addition, this application is designed to advance our understanding of the relationship between semaphorin structures and their inhibitory functions.
The specific aims are: 1) To identify elements of the activation domain of semaphorin 3A using several complementary approaches including chimeric proteins, deletion analysis, point mutations, inhibitory peptides and blocking antibodies. 2) To develop a reagent which inhibits all secreted semaphorins. This strategy may allow identification of novel biological roles for semaphorins since multiple secreted semaphorins may participate in each function and compensate for each other. 3) To examine whether secreted semaphorins contribute to regeneration failure within the adult spinal cord. This work will improve our understanding of the structure function relationship of the secreted semaphorins. This work should also advance our knowledge of the response to injury in the adult central nervous system.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
Eunice Kennedy Shriver National Institute of Child Health & Human Development (NICHD)
Type
Research Project (R01)
Project #
5R01HD038533-02
Application #
6388207
Study Section
Special Emphasis Panel (ZRG1-MDCN-7 (01))
Program Officer
Nitkin, Ralph M
Project Start
2000-07-01
Project End
2005-04-30
Budget Start
2001-05-01
Budget End
2002-04-30
Support Year
2
Fiscal Year
2001
Total Cost
$269,325
Indirect Cost

  Institution

Name
Massachusetts General Hospital
Department
Type
DUNS #
City
Boston
State
MA
Country
United States
Zip Code
02199

  Publications

Ben-Zvi, Ayal; Yagil, Zohar; Hagalili, Yamit et al. (2006) Semaphorin 3A and neurotrophins: a balance between apoptosis and survival signaling in embryonic DRG neurons. J Neurochem 96:585-97
Seijffers, Rhona; Woolf, Clifford J (2004) Utilization of an HSV-based amplicon vector encoding the axonal marker hPLAP to follow neurite outgrowth in cultured DRG neurons. J Neurosci Methods 132:169-76
Bloechlinger, Stefan; Karchewski, Laurie A; Woolf, Clifford J (2004) Dynamic changes in glypican-1 expression in dorsal root ganglion neurons after peripheral and central axonal injury. Eur J Neurosci 19:1119-32
Samad, Tarek A; Srinivasan, Ashok; Karchewski, Laurie A et al. (2004) DRAGON: a member of the repulsive guidance molecule-related family of neuronal- and muscle-expressed membrane proteins is regulated by DRG11 and has neuronal adhesive properties. J Neurosci 24:2027-36
Griffin, Robert S; Mills, Charles D; Costigan, Michael et al. (2003) Exploiting microarrays to reveal differential gene expression in the nervous system. Genome Biol 4:105
Costigan, Michael; Befort, Katia; Karchewski, Laurie et al. (2002) Replicate high-density rat genome oligonucleotide microarrays reveal hundreds of regulated genes in the dorsal root ganglion after peripheral nerve injury. BMC Neurosci 3:16
Benn, Susanna C; Perrelet, Daniel; Kato, Ann C et al. (2002) Hsp27 upregulation and phosphorylation is required for injured sensory and motor neuron survival. Neuron 36:45-56