A Unifying Genetic Model for Facioscapulohumeral Muscular Dystrophy

Richard J.L.F. Lemmers(Leiden University Medical Center), Patrick J. van der Vliet(Leiden University Medical Center), Rinse Klooster(Leiden University Medical Center), Sabrina Sacconi(Centre National de la Recherche Scientifique), Pilar Camaño(Instituto de Salud Carlos III), Johannes G. Dauwerse(Leiden University Medical Center), Lauren Snider(Fred Hutch Cancer Center), Kirsten R. Straasheijm(Leiden University Medical Center), G J van Ommen(Leiden University Medical Center), George W. Padberg(Radboud University Nijmegen), Daniel G. Miller(University of Washington), Stephen J. Tapscott(Fred Hutch Cancer Center), Rabi Tawil(University of Rochester Medical Center), Rune R. Frants(Leiden University Medical Center), Silvère M. van der Maarel(Leiden University Medical Center)
Science
August 19, 2010
10.1126/science.1189044
Cited by 777Open Access
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Abstract

Facioscapulohumeral muscular dystrophy (FSHD) is a common form of muscular dystrophy in adults that is foremost characterized by progressive wasting of muscles in the upper body. FSHD is associated with contraction of D4Z4 macrosatellite repeats on chromosome 4q35, but this contraction is pathogenic only in certain "permissive" chromosomal backgrounds. Here, we show that FSHD patients carry specific single-nucleotide polymorphisms in the chromosomal region distal to the last D4Z4 repeat. This FSHD-predisposing configuration creates a canonical polyadenylation signal for transcripts derived from DUX4, a double homeobox gene of unknown function that straddles the last repeat unit and the adjacent sequence. Transfection studies revealed that DUX4 transcripts are efficiently polyadenylated and are more stable when expressed from permissive chromosomes. These findings suggest that FSHD arises through a toxic gain of function attributable to the stabilized distal DUX4 transcript.

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