Disease Models & Mechanisms (May 2011)

Noonan syndrome gain-of-function mutations in NRAS cause zebrafish gastrulation defects

  • Vincent Runtuwene,
  • Mark van Eekelen,
  • John Overvoorde,
  • Holger Rehmann,
  • Helger G. Yntema,
  • Willy M. Nillesen,
  • Arie van Haeringen,
  • Ineke van der Burgt,
  • Boudewijn Burgering,
  • Jeroen den Hertog

DOI
https://doi.org/10.1242/dmm.007112
Journal volume & issue
Vol. 4, no. 3
pp. 393 – 399

Abstract

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SUMMARY Noonan syndrome is a relatively common developmental disorder that is characterized by reduced growth, wide-set eyes and congenital heart defects. Noonan syndrome is associated with dysregulation of the Ras–mitogen-activated-protein-kinase (MAPK) signaling pathway. Recently, two mutations in NRAS were reported to be associated with Noonan syndrome, T50I and G60E. Here, we report a mutation in NRAS, resulting in an I24N amino acid substitution, that we identified in an individual bearing typical Noonan syndrome features. The I24N mutation activates N-Ras, resulting in enhanced downstream signaling. Expression of N-Ras-I24N, N-Ras-G60E or the strongly activating mutant N-Ras-G12V, which we included as a positive control, results in developmental defects in zebrafish embryos, demonstrating that these activating N-Ras mutants are sufficient to induce developmental disorders. The defects in zebrafish embryos are reminiscent of symptoms in individuals with Noonan syndrome and phenocopy the defects that other Noonan-syndrome-associated genes induce in zebrafish embryos. MEK inhibition completely rescued the activated N-Ras-induced phenotypes, demonstrating that these defects are mediated exclusively by Ras-MAPK signaling. In conclusion, mutations in NRAS from individuals with Noonan syndrome activated N-Ras signaling and induced developmental defects in zebrafish embryos, indicating that activating mutations in NRAS cause Noonan syndrome.