A small peptide promotes EphA2 kinase-dependent signaling by stabilizing EphA2 dimers

The EphA2 receptor tyrosine kinase is known to promote cancer cell malignancy in the absence of activation by ephrin ligands. This behavior depends on high EphA2 phosphorylation on Ser897 and low tyrosine phosphorylation, resulting in increased cell migration and invasiveness. We have previously sho...

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Published inBiochimica et biophysica acta Vol. 1860; no. 9; pp. 1922 - 1928
Main Authors Singh, Deo R., Pasquale, Elena B., Hristova, Kalina
Format Journal Article
LanguageEnglish
Published Netherlands Elsevier B.V 01.09.2016
Subjects
Cell Line
cell movement
Cell Movement - physiology
dimerization
Ephrin-A2 - metabolism
Ephrins - metabolism
HEK293 Cells
Humans
Ligands
neoplasms
Peptides - metabolism
phosphorylation
Phosphorylation - physiology
plasma membrane
Protein Binding - physiology
Protein Multimerization - physiology
receptor protein-tyrosine kinase
Receptor, EphA2 - metabolism
Signal Transduction - physiology
tyrosine
Western blotting
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Summary:The EphA2 receptor tyrosine kinase is known to promote cancer cell malignancy in the absence of activation by ephrin ligands. This behavior depends on high EphA2 phosphorylation on Ser897 and low tyrosine phosphorylation, resulting in increased cell migration and invasiveness. We have previously shown that EphA2 forms dimers in the absence of ephrin ligand binding, and that dimerization of unliganded EphA2 can decrease EphA2 Ser897 phosphorylation. We have also identified a small peptide called YSA, which binds EphA2 and competes with the naturally occurring ephrin ligands. Here, we investigate the effect of YSA on EphA2 dimer stability and EphA2 function using quantitative FRET techniques, Western blotting, and cell motility assays. We find that the YSA peptide stabilizes the EphA2 dimer, increases EphA2 Tyr phosphorylation, and decreases both Ser897 phosphorylation and cell migration. The experiments demonstrate that the small peptide ligand YSA reduces EphA2 Ser897 pro-tumorigenic signaling by stabilizing the EphA2 dimer. This work is a proof-of-principle demonstration that EphA2 homointeractions in the plasma membrane can be pharmacologically modulated to decrease the pro-tumorigenic signaling of the receptor. •Small peptide ligands are known to increase EphA2 tyrosine phosphorylation.•We show that the YSA peptide ligand stabilizes the EphA2 dimer.•The YSA peptide ligand reduces EphA2 Ser897 phosphorylation.•The YSA peptide ligand decreases cell migration.
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ISSN:0304-4165
0006-3002
1872-8006
DOI:10.1016/j.bbagen.2016.06.004