Abstract

Much attention has been focused recently on E (epithelial)-cadherin and its role in cell-cell adhesion and tumor invasiveness. Indeed, the vast majority (approximately 90%) of human tumors are of epithelial origin (carcinomas), and epithelial cell-cell adhesion is mediated primarily by E-cadherin. In approximately 50% of metastatic carcinomas, E-cadherin expression is downregulated or lost altogether, and this is thought to figure prominently in tumor metastasis. The cytoplasmic regulators of E- cadherin, termed Catenins, have also been implicated in tumor progression: defects in these proteins may in fact explain metastatic events in the presence of apparently normal E-cadherin expression. Research in the applicant's laboratory has identified a novel 120 kDa catenin, designated p120, whose structural characteristics and direct binding to E-cadherin suggest a catenin-like role in cell-cell adhesion and signaling. Earlier studies characterized p120 as a protein tyrosine kinase (PTK) substrate whose phosphorylation correlates with Src-induced cell transformation. These observations, together with evidence linking the catenins to signaling pathways mediated by the Wnt oncoprotein and the adenomatous polyposis- coli (APC) tumor suppressor, suggest that chronic tyrosine phosphorylation of p120 contributes to the malignant phenotype by interfering with cadherin function or perhaps the Wnt- and APC-related signaling pathways. Thus, it becomes important to understand the role of p120 in PTK signaling and cadherin function. The proposed research seeks to determine the biological consequences of uncoupling cadherin and p120 functions by identifying and mutating the structural motifs in E-cadherin that specifically mediate its binding to p12O. In addition, the role of pl20 tyrosine phosphorylation in malignant cell behavior will be addressed by mapping the major phosphorylation site(s) on the pl2O molecule, with the long-range goal of mutating these sites and assaying the mutants for their effects on cell phenotype. Antibodies against the major pl20 phosphoepitopes will be used to dissect the signaling pathways relevant to pl20 and to determine the function of pl20 phosphorylation in cell-cell adhesion and signaling. Ultimately, the findings should contribute fresh insight into the role of this novel catenin in cadherin-mediated adhesion and signaling pathways and may suggest means by which one could suppress the metastatic changes associated with malignant tumors, including breast carcinoma.

  Funding Agency

Agency
National Institute of Health (NIH)
Institute
National Cancer Institute (NCI)
Type
Research Project (R01)
Project #
5R01CA055724-08
Application #
2654085
Study Section
Cellular Biology and Physiology Subcommittee 1 (CBY)
Program Officer
Mohla, Suresh
Project Start
1992-04-01
Project End
2001-01-31
Budget Start
1998-02-01
Budget End
1999-01-31
Support Year
8
Fiscal Year
1998
Total Cost
Indirect Cost

  Institution

Name
Vanderbilt University Medical Center
Department
Anatomy/Cell Biology
Type
Schools of Medicine
DUNS #
004413456
City
Nashville
State
TN
Country
United States
Zip Code
37212

  Publications

Short, Sarah P; Kondo, Jumpei; Smalley-Freed, Whitney G et al. (2017) p120-Catenin is an obligate haploinsufficient tumor suppressor in intestinal neoplasia. J Clin Invest 127:4462-4476
Yu, Huapeng H; Dohn, Michael R; Markham, Nicholas O et al. (2016) p120-catenin controls contractility along the vertical axis of epithelial lateral membranes. J Cell Sci 129:80-94
Markham, Nicholas O; Doll, Caleb A; Dohn, Michael R et al. (2014) DIPA-family coiled-coils bind conserved isoform-specific head domain of p120-catenin family: potential roles in hydrocephalus and heterotopia. Mol Biol Cell 25:2592-603
Markham, Nicholas O; Cooper, Tracy; Goff, Matthew et al. (2012) Monoclonal antibodies to DIPA: a novel binding partner of p120-catenin isoform 1. Hybridoma (Larchmt) 31:246-54
Smith, Andrew L; Dohn, Michael R; Brown, Meredith V et al. (2012) Association of Rho-associated protein kinase 1 with E-cadherin complexes is mediated by p120-catenin. Mol Biol Cell 23:99-110
Naydenov, Nayden G; Brown, Bryan; Harris, Gianni et al. (2012) A membrane fusion protein ?SNAP is a novel regulator of epithelial apical junctions. PLoS One 7:e34320
Kurley, Sarah J; Bierie, Brian; Carnahan, Robert H et al. (2012) p120-catenin is essential for terminal end bud function and mammary morphogenesis. Development 139:1754-64
Smith, Andrew L; Friedman, David B; Yu, Huapeng et al. (2011) ReCLIP (reversible cross-link immuno-precipitation): an efficient method for interrogation of labile protein complexes. PLoS One 6:e16206
Smalley-Freed, Whitney G; Efimov, Andrey; Short, Sarah P et al. (2011) Adenoma formation following limited ablation of p120-catenin in the mouse intestine. PLoS One 6:e19880
Stairs, Douglas B; Bayne, Lauren J; Rhoades, Ben et al. (2011) Deletion of p120-catenin results in a tumor microenvironment with inflammation and cancer that establishes it as a tumor suppressor gene. Cancer Cell 19:470-83

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