ASC-1 Is a Cell Cycle Regulator Associated with Severe and Mild Forms of Myopathy.
Rocio Nur Villar QuilesFabio CaterviEva CabetRaul Juntas-MoralesCasie A GenettiTeresa GidaroAsuman KoparirAdnan YükselSandra CoppensNicolas DeconinckEmma Pierce-HoffmanXavière LornageJulien DurigneuxJocelyn LaporteJohn RenduNorma B RomeroAlan H BeggsLaurent ServaisMireille CosseeMontse OlivéJohann BöhmIsabelle Duband-GouletAna FerreiroPublished in: Annals of neurology (2019)
Our results expand the phenotypical and molecular spectrum of TRIP4-associated disease to include mild adult forms with or without cardiomyopathy, associate ASC-1 depletion with isolated primary muscle involvement, and establish TRIP4 as a causative gene for several congenital muscle diseases, including nemaline, core, centronuclear, and cytoplasmic-body myopathies. They also identify ASC-1 as a novel cell cycle regulator with a key role in cell proliferation, and underline transcriptional coregulation defects as a novel pathophysiological mechanism. ANN NEUROL 2020;87:217-232.