Proinflammatory secreted phospholipase A2 type IIA (sPLA-IIA) induces integrin activation through direct binding to a newly identified binding site (site 2) in integrins αvβ3, α4β1, and α5β1

  • J Biol Chem. 2015 Jan 2;290(1):259-71. doi: 10.1074/jbc.M114.579946.
Masaaki Fujita  1 Kan Zhu  2 Chitose K Fujita  3 Min Zhao  2 Kit S Lam  4 Mark J Kurth  5 Yoko K Takada  6 Yoshikazu Takada  7
Affiliations
  • 1. From the Departments of Dermatology and Biochemistry and Molecular Medicine, UC Davis School of Medicine, Sacramento, California 95817, Department of Clinical Immunology and Rheumatology, The Tazuke-Kofukai Medical Research Institute, Kitano Hospital, Osaka 530-8480, Japan.
  • 2. From the Departments of Dermatology and.
  • 3. Department of Clinical Immunology and Rheumatology, The Tazuke-Kofukai Medical Research Institute, Kitano Hospital, Osaka 530-8480, Japan.
  • 4. Biochemistry and Molecular Medicine, UC Davis School of Medicine, Sacramento, California 95817.
  • 5. Department of Chemistry, UC Davis, Davis, California 95616, and.
  • 6. From the Departments of Dermatology and Biochemistry and Molecular Medicine, UC Davis School of Medicine, Sacramento, California 95817.
  • 7. From the Departments of Dermatology and Biochemistry and Molecular Medicine, UC Davis School of Medicine, Sacramento, California 95817, [email protected].
Abstract

Integrins are activated by signaling from inside the cell (inside-out signaling) through global conformational changes of integrins. We recently discovered that fractalkine activates integrins in the absence of CX3CR1 through the direct binding of fractalkine to a ligand-binding site in the Integrin headpiece (site 2) that is distinct from the classical RGD-binding site (site 1). We propose that fractalkine binding to the newly identified site 2 induces activation of site 1 though conformational changes (in an allosteric mechanism). We reasoned that site 2-mediated activation of integrins is not limited to fractalkine. Human secreted Phospholipase A2 type IIA (sPLA2-IIA), a proinflammatory protein, binds to integrins αvβ3 and α4β1 (site 1), and this interaction initiates a signaling pathway that leads to cell proliferation and inflammation. Human sPLA2-IIA does not bind to M-type receptor very well. Here we describe that sPLA2-IIA directly activated purified soluble Integrin αvβ3 and transmembrane αvβ3 on the cell surface. This activation did not require catalytic activity or M-type receptor. Docking simulation predicted that sPLA2-IIA binds to site 2 in the closed-headpiece of αvβ3. A peptide from site 2 of Integrin β1 specifically bound to sPLA2-IIA and suppressed sPLA2-IIA-induced Integrin activation. This suggests that sPLA2-IIA activates αvβ3 through binding to site 2. sPLA2-IIA also activated integrins α4β1 and α5β1 in a site 2-mediated manner. We recently identified small compounds that bind to sPLA2-IIA and suppress integrin-sPLA2-IIA interaction (e.g. compound 21 (Cmpd21)). Cmpd21 effectively suppressed sPLA2-IIA-induced Integrin activation. These results define a novel mechanism of proinflammatory action of sPLA2-IIA through Integrin activation.

Keywords
Adhesion; Allosteric Regulation; Docking Simulation; Fractalkine; Inflammation; Integrin; Integrin Activation; Peptides; Secreted Phospholipase A2 Type IIA.