Structure and function of a vimentin-associated matrix adhesion in endothelial cells

M Gonzales, B Weksler, D Tsuruta, R D Goldman, K J Yoon, S B Hopkinson, F W Flitney, J C R Jones

Research output: Contribution to journalArticlepeer-review

Abstract

The alpha4 laminin subunit is a component of endothelial cell basement membranes. An antibody (2A3) against the alpha4 laminin G domain stains focal contact-like structures in transformed and primary microvascular endothelial cells (TrHBMECs and HMVECs, respectively), provided the latter cells are activated with growth factors. The 2A3 antibody staining colocalizes with that generated by alphav and beta3 integrin antibodies and, consistent with this localization, TrHBMECs and HMVECs adhere to the alpha4 laminin subunit G domain in an alphav beta3-integrin-dependent manner. The alphav beta3 integrin/2A3 antibody positively stained focal contacts are recognized by vinculin antibodies as well as by antibodies against plectin. Unusually, vimentin intermediate filaments, in addition to microfilament bundles, interact with many of the alphav beta3 integrin-positive focal contacts. We have investigated the function of alpha4-laminin and alphav beta3-integrin, which are at the core of these focal contacts, in cultured endothelial cells. Antibodies against these proteins inhibit branching morphogenesis of TrHBMECs and HMVECs in vitro, as well as their ability to repopulate in vitro wounds. Thus, we have characterized an endothelial cell matrix adhesion, which shows complex cytoskeletal interactions and whose assembly is regulated by growth factors. Our data indicate that this adhesion structure may play a role in angiogenesis.

Original languageEnglish
Pages (from-to)85-100
Number of pages16
JournalMolecular Biology of the Cell
Volume12
Issue number1
DOIs
Publication statusPublished - 1 Jan 2001

Keywords

  • LAMININ ALPHA-CHAINS
  • INTEGRIN ALPHA(V)BETA(3)
  • ALPHA(6)BETA(4) INTEGRIN
  • EPITHELIAL-CELLS
  • EXPRESSION
  • HEMIDESMOSOMES
  • GROWTH
  • IDENTIFICATION
  • ANGIOGENESIS
  • CYTOSKELETON

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