Scientific Reports (Jun 2018)

NCAM2 Fibronectin type-III domains form a rigid structure that binds and activates the Fibroblast Growth Factor Receptor

  • Kim Krighaar Rasmussen,
  • Maria Hansen Falkesgaard,
  • Malene Winther,
  • Nikolaj Kulahin Roed,
  • Christine Louise Quistgaard,
  • Marie Nygaard Teisen,
  • Sofie Marie Edslev,
  • David Leander Petersen,
  • Ali Aljubouri,
  • Claus Christensen,
  • Peter Waaben Thulstrup,
  • Leila Lo Leggio,
  • Kaare Teilum,
  • Peter Schledermann Walmod

DOI
https://doi.org/10.1038/s41598-018-27089-7
Journal volume & issue
Vol. 8, no. 1
pp. 1 – 13

Abstract

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Abstract NCAM1 and NCAM2 have ectodomains consisting of 5 Ig domains followed by 2 membrane-proximal FnIII domains. In this study we investigate and compare the structures and functions of these FnIII domains. The NCAM1 and -2 FnIII2 domains both contain a Walker A motif. In NCAM1 binding of ATP to this motif interferes with NCAM1 binding to FGFR. We obtained a structural model of the NCAM2 FnIII2 domain by NMR spectroscopy, and by titration with an ATP analogue we show that the NCAM2 Walker A motif does not bind ATP. Small angle X-ray scattering (SAXS) data revealed that the NCAM2 FnIII1-2 double domain exhibits a very low degree of flexibility. Moreover, recombinant NCAM2 FnIII domains bind FGFR in vitro, and the FnIII1-2 double domain induces neurite outgrowth in a concentration-dependent manner through activation of FGFR. Several synthetic NCAM1-derived peptides induce neurite outgrowth via FGFR. Only 2 of 5 peptides derived from similar regions in NCAM2 induce neurite outgrowth, but the most potent of these peptides stimulates neurite outgrowth through FGFR-dependent activation of the Ras-MAPK pathway. These results reveal that the NCAM2 FnIII domains form a rigid structure that binds and activates FGFR in a manner related to, but different from NCAM1.