Methylation hotspots evidenced by deep sequencing in patients with facioscapulohumeral dystrophy and mosaicism.

Stéphane RocheCamille DionNatacha BroucqsaultCamille LaberthonnièreMarie-Cécile GaillardJérôme D RobinArnaud LagardeFrancesca PuppoCatherine VovanCharlene ChaixEmmanuelle Salort CampanaShahram AttarianMarc BartoliRafaelle BernardKarine NguyenFrédérique Magdinier

Published in: Neurology. Genetics (2019)

Altogether, our approach offers a new high throughput tool for estimation of the D4Z4 methylation level in the different subcategories of patients having FSHD. This methodology allows for a comprehensive and discriminative analysis of different regions along the macrosatellite repeat and identification of focal regions or CpG sites differentially methylated in patients with FSHD1 and FSHD2 but also complex cases such as those presenting mosaicism.

Keyphrases

high throughput
dna methylation
end stage renal disease
newly diagnosed
chronic kidney disease
ejection fraction
genome wide
single cell
prognostic factors
peritoneal dialysis
early onset
patient reported outcomes
patient reported