International Journal of Molecular Sciences (Oct 2022)

The PSI Domain of the MET Oncogene Encodes a Functional Disulfide Isomerase Essential for the Maturation of the Receptor Precursor

  • Dogus Murat Altintas,
  • Simona Gallo,
  • Cristina Basilico,
  • Marina Cerqua,
  • Alessio Bocedi,
  • Annapia Vitacolonna,
  • Orsola Botti,
  • Elena Casanova,
  • Ilaria Rancati,
  • Chiara Milanese,
  • Sara Notari,
  • Giorgia Gambardella,
  • Giorgio Ricci,
  • Pier Giorgio Mastroberardino,
  • Carla Boccaccio,
  • Tiziana Crepaldi,
  • Paolo Maria Comoglio

DOI
https://doi.org/10.3390/ijms232012427
Journal volume & issue
Vol. 23, no. 20
p. 12427

Abstract

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The tyrosine kinase receptor encoded by the MET oncogene has been extensively studied. Surprisingly, one extracellular domain, PSI, evolutionary conserved between plexins, semaphorins, and integrins, has no established function. The MET PSI sequence contains two CXXC motifs, usually found in protein disulfide isomerases (PDI). Using a scrambled oxidized RNAse enzymatic activity assay in vitro, we show, for the first time, that the MET extracellular domain displays disulfide isomerase activity, abolished by PSI domain antibodies. PSI domain deletion or mutations of CXXC sites to AXXA or SXXS result in a significant impairment of the cleavage of the MET 175 kDa precursor protein, abolishing the maturation of α and β chains, of, respectively, 50 kDa and 145 kDa, disulfide-linked. The uncleaved precursor is stuck in the Golgi apparatus and, interestingly, is constitutively phosphorylated. However, no signal transduction is observed as measured by AKT and MAPK phosphorylation. Consequently, biological responses to the MET ligand—hepatocyte growth factor (HGF)—such as growth and epithelial to mesenchymal transition, are hampered. These data show that the MET PSI domain is functional and is required for the maturation, surface expression, and biological functions of the MET oncogenic protein.

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