Abstract

During development, neurons find and synapse with one another in a remarkably precise way. How the nervous system becomes properly """"""""wired"""""""" during development is one of the major unsolved problems in biology. The unfolding of neuronal specificity involves a series of highly specific recognition events between individual neurons. The long term goal of this research program is to understand the cellular and molecular basis of cell recognition during neuronal development. Extensive cellular studies in the grasshopper embryo have shown that individual growth cones express selective affinities for particular axonal surfaces, and that these specificities give rise to the stereotyped patterns of selective fasciculation. Experimental results have suggested that many different molecules are differentially expressed on the surfaces of embryonic growth cones and axon fascicles. Monoclonal antibodies (MAbs) have revealed cell surface antigens whose temporal and spatial expression in the embryo corelate with these predictions. Whereas the grasshopper embryo is an excellent model system for a cellular analysis of neuronal development, the Drosophila embryo has obvious attributes for a molecular genetic analysis. Recent studies have shown that the early Drosophila embryo is a minature replica of the grasshopper embryo in terms of its identified neurons, their growth cones, and their selective fasciculation choices, thus opening the way for a combined cellualr and molecular genetic analysis of cell recognition. This proposal is to study the molecular basis of cell recognition during neuronal development in the Drosophila embryo.
The specific aims are (i) to isolate cDNA clones encoding molecules expressed on specific subsets of embryonic neurons early in development; (ii) to analyze the structure, distribution, and localization of the mRNAs and proteins they encode; and (iii) to understand the function of these surface molecules during neuronal development. The cDNA clones will be isolated by subtraction cDNA cloning, experssion cDNA cloning using specific MAbs, and/or synthetic oligonucleotide probes to amino acid sequences of purified antigens. The molecules will be characterized using recombinant DNA techniques, in situ hybridization, antibodies generated against their encoded proteins, primary cell cultures, and transfected cell lines. The function of these molecules will be studied using genetic analysis, gene fusions, and gene transformation techniques.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS018366-05
Application #
3398404
Study Section
Neurology C Study Section (NEUC)
Project Start
1982-06-01
Project End
1992-05-31
Budget Start
1986-06-01
Budget End
1987-05-31
Support Year
5
Fiscal Year
1986
Total Cost
Indirect Cost

  Institution

Name
Stanford University
Department
Type
Schools of Arts and Sciences
DUNS #
800771545
City
Stanford
State
CA
Country
United States
Zip Code
94305

  Publications

Hu, Hailan; Li, Ming; Labrador, Juan-Pablo et al. (2005) Cross GTPase-activating protein (CrossGAP)/Vilse links the Roundabout receptor to Rac to regulate midline repulsion. Proc Natl Acad Sci U S A 102:4613-8
Godenschwege, Tanja A; Simpson, Julie H; Shan, Xiaoliang et al. (2002) Ectopic expression in the giant fiber system of Drosophila reveals distinct roles for roundabout (Robo), Robo2, and Robo3 in dendritic guidance and synaptic connectivity. J Neurosci 22:3117-29
Kramer, S G; Kidd, T; Simpson, J H et al. (2001) Switching repulsion to attraction: changing responses to slit during transition in mesoderm migration. Science 292:737-40
Pipes, G C; Lin, Q; Riley, S E et al. (2001) The Beat generation: a multigene family encoding IgSF proteins related to the Beat axon guidance molecule in Drosophila. Development 128:4545-52
Simpson, J H; Bland, K S; Fetter, R D et al. (2000) Short-range and long-range guidance by Slit and its Robo receptors: a combinatorial code of Robo receptors controls lateral position. Cell 103:1019-32
Bashaw, G J; Kidd, T; Murray, D et al. (2000) Repulsive axon guidance: Abelson and Enabled play opposing roles downstream of the roundabout receptor. Cell 101:703-15
Simpson, J H; Kidd, T; Bland, K S et al. (2000) Short-range and long-range guidance by slit and its Robo receptors. Robo and Robo2 play distinct roles in midline guidance. Neuron 28:753-66
Kidd, T; Bland, K S; Goodman, C S (1999) Slit is the midline repellent for the robo receptor in Drosophila. Cell 96:785-94
Bashaw, G J; Goodman, C S (1999) Chimeric axon guidance receptors: the cytoplasmic domains of slit and netrin receptors specify attraction versus repulsion. Cell 97:917-26
Kidd, T; Brose, K; Mitchell, K J et al. (1998) Roundabout controls axon crossing of the CNS midline and defines a novel subfamily of evolutionarily conserved guidance receptors. Cell 92:205-15

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