4.7 Article

NHERF2 is crucial in ERM phosphorylation in pulmonary endothelial cells

Journal

CELL COMMUNICATION AND SIGNALING
Volume 11, Issue -, Pages -

Publisher

BMC
DOI: 10.1186/1478-811X-11-99

Keywords

Endothelial cells; Angiogenesis; ERM proteins; NHERF2

Categories

Funding

  1. Hungarian Science Research Fund [CNK80709]
  2. UD Faculty of Medicine Research Fund (University of Debrecen)
  3. Hungarian Social Renewal Operational Program [TAMOP-4.2.2/B-10/1-2010-0024, TAMOP-4.2.2.A-11/1/KONV-2012-0025]
  4. European Union
  5. State of Hungary
  6. European Social Fund [TAMOP 4.2.4.A/2-11/1-2012-0001]

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Background: EBP50 and NHERF2 adaptor proteins are incriminated in various signaling pathways of the cell. They can bind ERM proteins and mediate ERM-membrane protein interactions. Results: Binding of ERM to EBP50 and NHERF2 was compared in pulmonary artery endothelial cells by immunoprecipitation. NHERF2 associates with all three ERM, but EBP50 appeared to be a weak binding partner if at all. Furthermore, we detected co-localization of NHERF2 and phospho-ERM at the cell membrane and in the filopodia of dividing cells. Silencing of NHERF2 prevented agonist or angiogenesis induced phosphorylation of ERM, while overexpression of the adaptor elevated the phosphorylation level of ERM, likely catalyzed by Rho kinase 2, which co-immunoprecipitated with NHERF2/ERM in control EC, but did not bind to ERM in NHERF2 depleted cells. Dependence of ERM phosphorylation on NHERF2 was also shown in Matrigel tube formation assay, and NHERF2 was proved to be important in angiogenesis as well. Furthermore, when NHERF2 was depleted or cells were overexpressing a mutant form of NHERF2 unable to bind ERM, we found attenuated cell attachment with ECIS measurements, while it was supported by overexpression of wild type NHERF2. Conclusions: Pivotal role of NHERF2 in the phosphorylation process of ERM in pulmonary artery endothelial cells is shown. We propose that NHERF2 provides a common anchoring surface for ERM and Rho kinase 2. Our results demonstrate the essential role of NHERF2 in endothelial cell adhesion/migration and angiogenesis.

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