Abstract

Members of the Wnt gene family are related to the proto-oncogene Wnt-1 and the Drosophila segment polarity gene wingless. Wnts are thought to be secreted proteins acting during vertebrate embryonic development in a paracrine or autocrine fashion to activate receptors on target cells. While the functional significance, receptors, and mechanisms of Wnt-signal transduction are largely unknown, it is thought that Wnts are transiently expressed in localized tissues of embryos, and that they play an important role in intercellular communication involved in pattern formation. Supporting this, deregulation of the timing and spatial expression of the neural-specific Wnt-1 causes pattern defects in Xenopus embryos, and deletion of these genes in mouse results in midbrain and hindbrain defects. The current project will directly test the hypothesis that the Wnt gene family plays an essential role in embryonic pattern formation in vertebrates and will investigate the signal transduction pathway involved in intercellular signalling by Wnts. The zebrafish (Brachydanio rerio) will be used for these studies, as it offers genetic analysis as well as accessible early embryonic development. The specific goals follow: 1. The Wnt gene family will be cloned by amplification of Wnt sequences with degenerate oligonucleotide primers, followed by cDNA library screening to isolate the full coding sequences. 2. cDNAs from Aim 1 will be employed for RNA blot analysis and for in situ hybridization while, in parallel, antisera will be developed and employed in immunocytochemistry at the light and EM level. These studies will establish the temporal and spatial pattern of expression of each Wnt. 3. Genetic approaches will be employed to alter Wnt expression, or interfere with Wnt function. Analysis of the mutant phenotypes may reveal insights into the roles of Wnts in development. 4. The pathways by which Wnts signal spatial information between cells will be studied by examining whether deregulation of Wnt patterns of expression affects gap junctional communication and known second messenger systems and by pursuing zebrafish homologues of genes which operate in the Wnt pathway in Drosophila. Collectively, these studies will directly test the functions and mechanisms of actions of newly discovered signalling polypeptides which may, when aberrantly expressed, be involved in birth defects and transformation of cells.

  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 #
5R01HD029360-03
Application #
2201758
Study Section
Molecular Biology Study Section (MBY)
Project Start
1992-08-01
Project End
1997-06-30
Budget Start
1994-07-01
Budget End
1995-06-30
Support Year
3
Fiscal Year
1994
Total Cost
Indirect Cost

  Institution

Name
University of Washington
Department
Pharmacology
Type
Schools of Medicine
DUNS #
135646524
City
Seattle
State
WA
Country
United States
Zip Code
98195

  Publications

Lekven, A C; Thorpe, C J; Waxman, J S et al. (2001) Zebrafish wnt8 encodes two wnt8 proteins on a bicistronic transcript and is required for mesoderm and neurectoderm patterning. Dev Cell 1:103-14
Miller, J R; Rowning, B A; Larabell, C A et al. (1999) Establishment of the dorsal-ventral axis in Xenopus embryos coincides with the dorsal enrichment of dishevelled that is dependent on cortical rotation. J Cell Biol 146:427-37
Ungar, A R; Helde, K A; Moon, R T (1998) Production of androgenetic haploids in zebrafish with ultraviolet light. Mol Mar Biol Biotechnol 7:320-6
Du, S J; Devoto, S H; Westerfield, M et al. (1997) Positive and negative regulation of muscle cell identity by members of the hedgehog and TGF-beta gene families. J Cell Biol 139:145-56
Larabell, C A; Torres, M; Rowning, B A et al. (1997) Establishment of the dorso-ventral axis in Xenopus embryos is presaged by early asymmetries in beta-catenin that are modulated by the Wnt signaling pathway. J Cell Biol 136:1123-36
Pearson, D S; Kulyk, W M; Kelly, G M et al. (1996) Cloning and characterization of a cDNA encoding the collagen-binding stress protein hsp47 in zebrafish. DNA Cell Biol 15:263-72
Yost, C; Torres, M; Miller, J R et al. (1996) The axis-inducing activity, stability, and subcellular distribution of beta-catenin is regulated in Xenopus embryos by glycogen synthase kinase 3. Genes Dev 10:1443-54
Torres, M A; Yang-Snyder, J A; Purcell, S M et al. (1996) Activities of the Wnt-1 class of secreted signaling factors are antagonized by the Wnt-5A class and by a dominant negative cadherin in early Xenopus development. J Cell Biol 133:1123-37
Ungar, A R; Kelly, G M; Moon, R T (1995) Wnt4 affects morphogenesis when misexpressed in the zebrafish embryo. Mech Dev 52:153-64
Kelly, G M; Erezyilmaz, D F; Moon, R T (1995) Induction of a secondary embryonic axis in zebrafish occurs following the overexpression of beta-catenin. Mech Dev 53:261-73

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