Abstract

Axonal outgrowth is guided by molecular cues deposited in trails, or spatial gradients, on the extracellular matrix. Growth cones navigating these pathways must express the appropriate receptors in the proper sequence. Thus, the final patterning of axon tracts reflects genetic programs that control the expression of directional cues and neuronal receptors. The major goals are to 1) identify the cellular substrata that support axonal outgrowth, 2) characterize the spatial patterning of directional cues that guide axonal outgrowth, 3) identify the neuronal receptors and their temporal programming, and 4) learn how localized receptor activation steers growth cone direction. Using the genetic model Caenorhabditis elegans, the applicant has identified three genes whose products guide axonal outgrowth, unc-6, unc-5, and unc-40. UNC-6 is a laminin-related matrix protein secreted by epidermal cells (neuroglia), that, like its vertebrate homologues the netrins, guides the dorsal and ventral migration of axons. UNC-5, a transmembrane receptor for UNC-6, guides dorsal migration, and UNC-40, a DCC homologue, is necessary for ventral migration. In the proposed experiments, the localization of UNC-6, UNC-5, and UNC-40, and the dependence of their pattern on other genotypes will be studied. A gene that interacts with unc-6, adn-2, and a related gene adn-1, will be molecularly characterized. The experimental plan also investigates how a navigational program intrinsic to motile cells, the wingless signal transduction pathway, controls the polarity of guidance receptor expression during migrations. Disheveled, which is a key player in the wingless pathway is encoded by the mig-5 gene in C. elegans. Genetic interactions between UNC-40 and the wingless pathway will be studied by examining mig-5 expression in unc-40 mutants. UNC-6/netrin, UNC-40/DCC, and the wingless pathway are phyletically ancient and highly conserved in structure. Therefore, analysis of their roles in regulating axon and cell migration during normal and mutant development may aid the rational design of molecular therapies for the repopulation of axon tracts severed by injury or destroyed by disease.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Institute of Neurological Disorders and Stroke (NINDS)
Type
Research Project (R01)
Project #
5R01NS026295-10
Application #
6126217
Study Section
Neurology C Study Section (NEUC)
Program Officer
Chiu, Arlene Y
Project Start
1988-08-01
Project End
2001-11-30
Budget Start
1999-12-01
Budget End
2000-11-30
Support Year
10
Fiscal Year
2000
Total Cost
$302,578
Indirect Cost

  Institution

Name
Johns Hopkins University
Department
Biology
Type
Schools of Arts and Sciences
DUNS #
045911138
City
Baltimore
State
MD
Country
United States
Zip Code
21218

  Publications

Walston, Timothy; Guo, Chaobo; Proenca, Rui et al. (2006) mig-5/Dsh controls cell fate determination and cell migration in C. elegans. Dev Biol 298:485-97
Kao, Gautam; Huang, Cheng-chen; Hedgecock, Edward M et al. (2006) The role of the laminin beta subunit in laminin heterotrimer assembly and basement membrane function and development in C. elegans. Dev Biol 290:211-9
Huang, Cheng-Chen; Hall, David H; Hedgecock, Edward M et al. (2003) Laminin alpha subunits and their role in C. elegans development. Development 130:3343-58
Kipreos, E T; Gohel, S P; Hedgecock, E M (2000) The C. elegans F-box/WD-repeat protein LIN-23 functions to limit cell division during development. Development 127:5071-82
Antebi, A; Yeh, W H; Tait, D et al. (2000) daf-12 encodes a nuclear receptor that regulates the dauer diapause and developmental age in C. elegans. Genes Dev 14:1512-27
Buechner, M; Hall, D H; Bhatt, H et al. (1999) Cystic canal mutants in Caenorhabditis elegans are defective in the apical membrane domain of the renal (excretory) cell. Dev Biol 214:227-41
Antebi, A; Culotti, J G; Hedgecock, E M (1998) daf-12 regulates developmental age and the dauer alternative in Caenorhabditis elegans. Development 125:1191-205
Chan, S S; Zheng, H; Su, M W et al. (1996) UNC-40, a C. elegans homolog of DCC (Deleted in Colorectal Cancer), is required in motile cells responding to UNC-6 netrin cues. Cell 87:187-95
Wadsworth, W G; Hedgecock, E M (1996) Hierarchical guidance cues in the developing nervous system of C. elegans. Bioessays 18:355-62
Kipreos, E T; Lander, L E; Wing, J P et al. (1996) cul-1 is required for cell cycle exit in C. elegans and identifies a novel gene family. Cell 85:829-39

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