Abstract

During neural development, a population of morphologically homogenous, mitotically active precursor cells gives rise to all the neuronal and glial cells of the adult cerebral cortex. Postmitotic neurons extend processes by which they migrate to their adult positions and begin the elaboration of axonal and dendritic arbors. To understand the molecular events that permit a cell to assume neuronal properties, we previously used 2- dimensional gel electrophoresis to identify 15 proteins that are differentially regulated over the course of corticogenesis. One of these, TOAD-64, is a 64,000 dalton protein that is up regulated nearly 7-fold over the course of late embryonic cortical development and is subsequently down regulated during postnatal life. The sequence of a full length cDNA of TOAD-64 is homologous to the unc-33 gene from C. elegans, mutations in which lead to defective patterns of axon outgrowth. Several lines of evidence suggest that TOAD-64 may, similarly, play a role in axonogenesis in the rodent. First, TOAD-64 is re-expressed in adult motor neurons as they extend axons following a peripheral nerve lesion. Second, TOAD-64 expression increases coincident with neuritogenesis in two cell lines, pC12 and p19. Finally, TOAD-64 protein is present at the most peripheral portions of the growth cone, in lamellipodia and filopodia. Together, these data support the possibility that TOAD-64 is part of the intracellular machinery by which growing neurons elaborate axons. The experiments proposed here are designed to further characterize TOAD-64 and will also address the possible functions of this new protein in neurite outgrowth.
The first aim i s to further characterize TOAD-64. A possible role for TOAD-64 in neuronal remodeling in the adult will be investigated. A new panel of antibodies to primate TOAD-64 will be generated to permit studies of early corticogenesis in the monkey. For studies of the mechanisms by which the TOAD-64 gene is regulated, a genomic clone will be isolated for future experiments to identify its regulatory sequences.
The second aim i s to determine the function of TOAD-64. We will explore the role TOAD-64 may play in axonogenesis by changing levels of protein expression in primary neuronal cultures and in two cell lines. To test whether TOAD-64 is required for a cell to elaborate neurites, antisense oligonucleotides will be used to reduce TOAD-64 expression in neurons in primary culture. We will also determine whether a reduction in TOAD-64 can alter the response of growth cones and neurites to repulsive substrates. To determine whether TOAD-64 is critical for the elaboration of neurites in PC12 and P19 cells, expression of TOAD-64 will be reduced or increased using stable transfection.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Program Projects (P01)
Project #
3P01NS022807-14S1
Application #
6112240
Study Section
Project Start
1999-03-01
Project End
2000-02-29
Budget Start
1998-10-01
Budget End
1999-09-30
Support Year
14
Fiscal Year
1999
Total Cost
Indirect Cost

  Institution

Name
Yale University
Department
Type
DUNS #
082359691
City
New Haven
State
CT
Country
United States
Zip Code
06520

  Publications

Quinn, Christopher C; Chen, Esteban; Kinjo, Tashi G et al. (2003) TUC-4b, a novel TUC family variant, regulates neurite outgrowth and associates with vesicles in the growth cone. J Neurosci 23:2815-23
Turner, Christopher P; Yan, Henglin; Schwartz, Michael et al. (2002) A1 adenosine receptor activation induces ventriculomegaly and white matter loss. Neuroreport 13:1199-204
Wasiak, S; Quinn, C C; Ritter, B et al. (2001) The Ras/Rac guanine nucleotide exchange factor mammalian Son-of-sevenless interacts with PACSIN 1/syndapin I, a regulator of endocytosis and the actin cytoskeleton. J Biol Chem 276:26622-8
Haydar, T F; Wang, F; Schwartz, M L et al. (2000) Differential modulation of proliferation in the neocortical ventricular and subventricular zones. J Neurosci 20:5764-74
Tong, X K; Hussain, N K; de Heuvel, E et al. (2000) The endocytic protein intersectin is a major binding partner for the Ras exchange factor mSos1 in rat brain. EMBO J 19:1263-71
Quinn, C C; Gray, G E; Hockfield, S (1999) A family of proteins implicated in axon guidance and outgrowth. J Neurobiol 41:158-64
Wang, F; Lidow, M S (1997) Alpha 2A-adrenergic receptors are expressed by diverse cell types in the fetal primate cerebral wall. J Comp Neurol 378:493-507
Redmond, L; Xie, H; Ziskind-Conhaim, L et al. (1997) Cues intrinsic to the spinal cord determine the pattern and timing of primary afferent growth. Dev Biol 182:205-18
Anton, E S; Cameron, R S; Rakic, P (1996) Role of neuron-glial junctional domain proteins in the maintenance and termination of neuronal migration across the embryonic cerebral wall. J Neurosci 16:2283-93
Fryer, H J; Hockfield, S (1996) The role of polysialic acid and other carbohydrate polymers in neural structural plasticity. Curr Opin Neurobiol 6:113-8

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