Metformin ameliorates core deficits in a mouse model of fragile X syndrome.

Ilse GantoisArkady KhoutorskyJelena PopicArgel Aguilar-VallesErika FreemantleRuifeng CaoVijendra SharmaTine Pooters Anmol NagpalAgnieszka SkaleckaVinh T TruongShane WiebeIsabelle A GrovesSeyed Mehdi JafarnejadClément ChapatElizabeth A McCullaghKarine GamacheKarim NaderJean-Claude Lacaille Christos G GkogkasNahum Sonenberg

Published in: Nature medicine (2017)

Fragile X syndrome (FXS) is the leading monogenic cause of autism spectrum disorders (ASD). Trinucleotide repeat expansions in FMR1 abolish FMRP expression, leading to hyperactivation of ERK and mTOR signaling upstream of mRNA translation. Here we show that metformin, the most widely used drug for type 2 diabetes, rescues core phenotypes in Fmr1-/y mice and selectively normalizes ERK signaling, eIF4E phosphorylation and the expression of MMP-9. Thus, metformin is a potential FXS therapeutic.

Keyphrases

mouse model
autism spectrum disorder
poor prognosis
type diabetes
cell proliferation
signaling pathway
binding protein
pi k akt
traumatic brain injury
intellectual disability
emergency department
glycemic control
healthcare
weight loss