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DOI: 10.1160/TH04-10-0680
Downregulation of vascular endothelial-cadherin expression is associated with an increase in vascular tumor growth and hemorrhagic complications
Financial support: This work was supported by Associazione Italiana per la Ricerca sul Cancro, the European community (QLRT-2001–02059; Integrated Project contract LSHG-CT-2004–503573; No EMAIN 502935; No E EVGN 503254;); Italian Ministry of Health, Special Project on Stem Cells (CS36 and CS39), Ministry of University and Scientific and Technological Research, CNR/MIUR (CNR.02.731. DEJA), MIUR/FIRB (RBNE01MAWA_009, RBNE01F8LT_007); Cofin 2003 (2003058397_04); and the Swiss National Science Foundation (grant no. 3100–064037.00 to MSP). L. Z. was supported by a fellowship from Fondazione Italiana per la Ricerca sul Cancro.Publication History
Received
20 October 2004
Accepted after revision
04 April 2005
Publication Date:
11 December 2017 (online)
Summary
The pathogenesis of vascular tumors such as angiosarcomas is poorly understood. Cadherin expression inversely correlates with tumor malignancy and the endothelial specific VE-cadherin is low or absent in angiosarcomas, suggesting an inhibitory role for this protein in tumor progression. In this paper we report that Pmy T VE-cadherin null (VEC null) endothelial cells form larger vascular tumors in nude mice when injected subcutaneously as compared to isogenic VE-cadherin positive (VEC pos) cells. This effect requires the association of β-catenin to VE-cadherin, since a VE-cadherin mutant lacking the domain responsible for β-catenin binding (Δβcat) cannot rescue the phenotype. In VEC null cells β-catenin is phosphorylated and partly degraded. N-cadherin is increased and detected at junctions. VEC null cells also present an altered fibrinolytic activity with increases in tPA, uPA, uPAR and a strong reduction in PAI-1, which may be correlated to the high incidence of abrupt hemorrhages in VEC null tumors. Overall, these data strongly suggest that downregulation of VE-cadherin in endothelial tumors may have important consequences for tumor growth and bleeding complications.