4.6 Article

Binding of CD157 Protein to Fibronectin Regulates Cell Adhesion and Spreading

Journal

JOURNAL OF BIOLOGICAL CHEMISTRY
Volume 289, Issue 22, Pages 15588-15601

Publisher

AMER SOC BIOCHEMISTRY MOLECULAR BIOLOGY INC
DOI: 10.1074/jbc.M113.535070

Keywords

Cell Adhesion; Cell Surface Receptor; Extracellular Matrix; Fibronectin; Membrane Protein; BST-1; CD157; Heparin-binding Domain

Funding

  1. Italian Association for Cancer Research [IG 11602]
  2. Italian Ministry for University and Scientific Research
  3. International Foundation for Research in Experimental Medicine
  4. Fondazione Umberto Veronesi

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CD157/BST-1 behaves both as an ectoenzyme and signaling receptor and is an important regulator of leukocyte trafficking and ovarian cancer progression. However, the molecular interactions underpinning the role of CD157 in these processes remain obscure. The biological functions of CD157 and its partnership with members of the integrin family prompted us to assume the existence of a direct interaction between CD157 and an unknown component of the extracellular matrix. Using solid-phase binding assays and surface plasmon resonance analysis, we demonstrated that CD157 binds fibronectin with high affinity within its heparin-binding domains 1 and 2. Furthermore, we found that CD157 binds to other extracellular matrix proteins containing heparin-binding domains. Finally, we proved that the CD157-fibronectin interaction occurs with living cells, where it elicits CD157-mediated cell responses. Indeed, knockdown of CD157 in Met-5A mesothelial cells changed their morphology and cytoskeleton organization and attenuated the activation of intracellular signaling pathways triggered by fibronectin. This led to impaired cell spreading and adhesion to selected extracellular matrix proteins. Collectively, these findings indicate a central role of CD157 in cell-extracellular matrix interactions and make CD157 an attractive therapeutic target in inflammation and cancer.

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