Noonan syndrome-associated biallelic LZTR1 mutations cause cardiac hypertrophy and vascular malformations in zebrafish.

Yu NakagamaNorihiko TakedaSeishi OgawaHiroyuki TakedaYoshiyuki FurutaniToshio NakanishiTatsuyuki SatoYoichiro HirataAkira OkaRyo Inuzuka

Published in: Molecular genetics & genomic medicine (2019)

Our novel zebrafish model phenocopied human recessive Noonan syndrome and supported the loss-of-function mechanism of disease-causing LZTR1 variants. The discovery of vascular malformations in mutants calls for the clinical follow-up of patients to monitor for its emergence. The model will serve as a novel platform for investigating the pathophysiology linking RAS/MAPK signaling to cardiac and vascular pathology.

Keyphrases

end stage renal disease
endothelial cells
newly diagnosed
ejection fraction
intellectual disability
high throughput
case report
small molecule
oxidative stress
prognostic factors
copy number
autism spectrum disorder