1. Endoglin overexpression modulates cellular morphology, migration, and adhesion of mouse fibroblasts
- Author
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Carmen Langa, Pedro Lastres, Ainhoa Letamendia, Angeles García-Pardo, Sonia Vera, Carmelo Bernabeu, Michelle Letarte, Mercedes Guerrero-Esteo, Maria Jose Perez-Alvarez, Luis López, Angels Fabra, Comisión Interministerial de Ciencia y Tecnología, CICYT (España), Comunidad de Madrid, European Commission, Lastres, Pedro, Letamendía, Ainhoa, Pérez-Álvarez, María José, Fabra, Àngels, García-Pardo, Angeles, Vera, Sonia, Letarte, Michelle, Bernabéu, Carmelo, Lastres, Pedro [0000-0002-5996-1426], Letamendía, Ainhoa [0000-0001-9232-8377], Pérez-Álvarez, María José [0000-0001-8334-8085], Fabra, Àngels [0000-0003-3288-523X], García-Pardo, Angeles [0000-0001-5577-2954], Vera, Sonia [0000-0002-4873-6098], Letarte, Michelle [0000-0002-5901-7582], and Bernabéu, Carmelo [0000-0002-1563-6162]
- Subjects
Histology ,Integrin ,Vascular Cell Adhesion Molecule-1 ,Receptors, Cell Surface ,Transfection ,HHT ,Pathology and Forensic Medicine ,Extracellular matrix ,Mice ,Receptors, Fibronectin ,Antigens, CD ,Cell Movement ,Laminin ,hemic and lymphatic diseases ,Plasminogen Activator Inhibitor 1 ,Cell Adhesion ,otorhinolaryngologic diseases ,Animals ,Humans ,Receptor ,Wound Healing ,Transfectants ,Microscopy, Confocal ,biology ,Endoglin ,Cell Biology ,General Medicine ,Fibroblasts ,Flow Cytometry ,Molecular biology ,Fibronectin ,TGF-ß ,biology.protein ,Collagen ,Wound healing ,Transforming growth factor - Abstract
10 p.-9 fig.-1 tab., Endoglin is the gene mutated in hereditary hemorrhagic telangiectasia type 1 (HHT1), a dominantly inherited vascular disorder. Endoglin glycoprotein is a component of the transforming growth factor type ß (TGF-ß) receptor system which is highly expressed by endothelial cells, and at lower levels on fibroblasts and smooth muscle cells, suggesting the involvement of these lineages in the HHT1 vascular dysplasia. Overexpression of endoglin in mouse NCTC929 fibroblasts led to decreased migration in chemotactic and wound healing assays, as well as changes in the cellular morphology. When plated on uncoated surfaces, endoglin transfectants formed intercellular clusters, endoglin being not specifically localized to the cell-cell junctions, but homogenously distributed on the cellular surface. Although the expression of α5ß1 integrin and of an activation epitope of ß1 integrin were unchanged, a polyclonal antibody to α5ß1 integrin was able to inhibit cluster formation, suggesting the involvement of integrin ligand/s. In fact, coating with fibronectin, laminin, or an RGD-containing 80 kDa fragment of fibronectin were able to prevent the cellular clustering. Furthermore, synthesis of plasminogen activator inhibitor 1 (PAI-1), and to a weak extent that of fibronectin, were inhibited in endoglin transfectants. Thus, the presence of endoglin in mouse NCTC929 fibroblasts is associated with reduced production of certain extracellular matrix (ECM) components, which might explain their altered morphology, migration and intercellular cluster formation., This work has been supported by grants from Camisión Interministerial de Ciencia yTecnología (CICYT-SAF97-0034 to C. Bernabéu, and CICYT-SAF97-0064-C03-02 to A. García-Pardo), Comunidad Autónoma de Madrid (CAM) and Biomed Program of the European Community (BMH4-CT95-0995 to C. Bernabéu).
- Published
- 1999
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