1. Urokinase receptor mediates lung fibroblast attachment and migration toward provisional matrix proteins through interaction with multiple integrins
- Author
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Qiang Ding, Kimberly E. White, Mitchell A. Olman, Tong H. Jin, Harold A. Chapman, Jerry E. Stewart, Candece L. Gladson, and Sha Zhu
- Subjects
Adult ,Pulmonary and Respiratory Medicine ,Integrins ,Physiology ,Plasmin ,Integrin ,Biology ,Receptors, Urokinase Plasminogen Activator ,Mice ,Cell Movement ,Fibrosis ,Physiology (medical) ,Pulmonary fibrosis ,Cell Adhesion ,medicine ,Animals ,Humans ,Vitronectin ,Receptor ,Fibroblast ,Lung ,Urokinase ,Extracellular Matrix Proteins ,Wound Healing ,Fibrinogen ,Articles ,Cell Biology ,Fibroblasts ,medicine.disease ,Fibronectins ,Cell biology ,Urokinase receptor ,Protein Subunits ,Protein Transport ,medicine.anatomical_structure ,Immunology ,biology.protein ,Cattle ,Cell Surface Extensions ,Collagen ,Protein Binding ,medicine.drug - Abstract
Fibroblasts from patients with pulmonary fibrosis express higher levels of the receptor for urokinase, and the extent of fibrosis in some animal models exhibits a dependence on the urokinase receptor. Recent observations have identified the urokinase receptor as a trans-interacting receptor with consequences on signaling and cell responses that vary depending on its interacting partner, the relative levels of expression, and the state of cellular transformation. We undertook this study to define the urokinase-type plasminogen activator cellular receptor (u-PAR)-integrin interactions and to determine the functional consequences of such interactions on normal human lung fibroblast attachment and migration. u-PAR colocalizes in lammelipodia/filopodia with relevant integrins that mediate fibroblast attachment and spreading on the provisional matrix proteins vitronectin, fibronectin, and collagens. Inhibitory antibody studies have revealed that human lung fibroblasts utilize αvβ5to attach to vitronectin, predominantly α5β1(and αvβ3) to attach to fibronectin, and α1β1, α2β1, and α3β1to attach to collagen. Blocking studies with α-integrin subunit decoy peptides and u-PAR neutralizing antibodies indicate that u-PAR modulates the integrin-mediated attachment to purified provisional matrix proteins, to anti-integrin antibodies, or to fibroproliferative lesions from fibrotic lungs. Furthermore, these decoy peptides blunt fibroblast spreading and migration. We show that u-PAR can interact with multiple α-integrins but with a preference for α3. Taken together, these data demonstrate that u-PAR may interact with multiple integrins in normal human lung fibroblasts thereby promoting attachment, spreading, and migration. Modulation of fibroblast invasion would be expected to lead to amelioration of fibroproliferative diseases of the lung.
- Published
- 2009
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