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The zebrafish HGF receptor met controls migration of myogenic progenitor cells in appendicular development.

Hanna NordNils DennhagHanna TydingerJonas von Hofsten
Published in: PloS one (2019)
The hepatocyte growth factor receptor C-met plays an important role in cellular migration, which is crucial for many developmental processes as well as for cancer cell metastasis. C-met has been linked to the development of mammalian appendicular muscle, which are derived from migrating muscle progenitor cells (MMPs) from within the somite. Mammalian limbs are homologous to the teleost pectoral and pelvic fins. In this study we used Crispr/Cas9 to mutate the zebrafish met gene and found that the MMP derived musculature of the paired appendages was severely affected. The mutation resulted in a reduced muscle fibre number, in particular in the pectoral abductor, and in a disturbed pectoral fin function. Other MMP derived muscles, such as the sternohyoid muscle and posterior hypaxial muscle were also affected in met mutants. This indicates that the role of met in MMP function and appendicular myogenesis is conserved within vertebrates.
Keyphrases
  • skeletal muscle
  • tyrosine kinase
  • growth factor
  • crispr cas
  • gene expression
  • transcription factor
  • dna methylation
  • copy number
  • oxidative stress
  • rectal cancer
  • binding protein