Telomere position effect regulates DUX4 in human facioscapulohumeral muscular dystrophy

Stadler, Guido; Rahimov, Fedik; King, Oliver D.; Chen, Jennifer C. J.; Robin, Jérôme D.; Wagner, Kathryn R.; Shay, Jerry W.; Emerson, Charles P.; Wright, Woodring E.

doi:10.1038/nsmb.2571

Cited by 99 publications

(108 citation statements)

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“…However, in a number of cases, the role of DUX4 remains unclear due to the complexity of its expression pattern (Dixit et al 2007;Snider et al 2010;Tassin et al 2013), low mRNA and protein abundance Ferreboeuf et al 2014), and the presence of DUX4 in unaffected individuals (Jones et al 2012;Broucqsault et al 2013). Thus, DUX4 might not be sufficient to explain the wide variability of the pathology, the muscle specificity and asymmetry, or the age-related onset suggesting that other factors are likely involved (Cabianca et al 2012;Caruso et al 2013;Stadler et al 2013;Mariot et al 2015;Puppo et al 2015).…”

Section: [Supplemental Materials Is Available For This Article]mentioning

confidence: 99%

“…Among them, we recently investigated the role of progressive telomere shortening in FSHD due to its age-related onset and because the genetic locus linked to the disease is only 25-50 kb from the Chromosome 4q telomere. Since telomeres are known to progressively shorten with increased cell turnover, we hypothesized that telomere proximity might contribute to the disease through telomere position effect (TPE) (Stadler et al 2013).…”

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confidence: 99%

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SORBS2transcription is activated by telomere position effect–over long distance upon telomere shortening in muscle cells from patients with facioscapulohumeral dystrophy

et al. 2015

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DNA is organized into complex three-dimensional chromatin structures, but how this spatial organization regulates gene expression remains a central question. These DNA/chromatin looping structures can range in size from 10-20 kb (enhancers/repressors) to many megabases during intra-and inter-chromosomal interactions. Recently, the influence of telomere length on chromatin organization prior to senescence has revealed the existence of long-distance chromatin loops that dictate the expression of genes located up to 10 Mb from the telomeres (Telomere Position Effect-Over Long Distances [TPE-OLD]). Here, we demonstrate the existence of a telomere loop at the 4q35 locus involving the sorbin and SH3 domain-containing protein 2 gene, SORBS2, a skeletal muscle protein using a modification of the chromosome conformation capture method. The loop reveals a cis-acting mechanism modifying SORBS2 transcription. The expression of this gene is altered by TPE-OLD in myoblasts from patients affected with the age-associated genetic disease, facioscapulohumeral muscular dystrophy (FSHD1A, MIM 158900). SORBS2 is expressed in FSHD myoblasts with short telomeres, while not detectable in FSHD myoblasts with long telomeres or in healthy myoblasts regardless of telomere length. This indicates that TPE-OLD may modify the regulation of the 4q35 locus in a pathogenic context. Upon differentiation, both FSHD and healthy myotubes express SORBS2, suggesting that SORBS2 is normally up-regulated by maturation/differentiation of skeletal muscle and is misregulated by TPE-OLD-dependent variegation in FSHD myoblasts. These findings provide additional insights for the complexity and age-related symptoms of FSHD.

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confidence: 99%

Section: [Supplemental Materials Is Available For This Article]mentioning

confidence: 99%

SORBS2transcription is activated by telomere position effect–over long distance upon telomere shortening in muscle cells from patients with facioscapulohumeral dystrophy

et al. 2015

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“…Comme la liaison de CTCF s'accompagne d'une augmentation de la densité locale d'H2A.Z [26], cela pourrait suggérer que, à l'instar de ce qui a été observé chez la levure [9], ce variant d'histone contribuerait également aux barrières subtélomériques humaines. L'importance de la présence de barrières naturelles contre la propagation de l'HC télomérique humaine a été à nouveau suggérée dans une étude récente décri-vant l'existence d'un TPE endogène dans le cas particulier de la dystrophie facio-scapulo-humérale ou myopathie FSH [27]. La myopathie FSH est associée à une contraction pathologique des répétitions D4Z4 subté-lomériques en 4q35, et à l'induction transcriptionnelle du locus DUX4 situé au sein de ces répétitions.…”

Section: L'effet De Position Télomérique Chez L'hommeunclassified

“…La dimérisation de molécules de CTCF pourrait être impliquée dans ce processus. Télomère HP1 HP1 HP1 HP1 HP1 HP1 HP1 HP1 HP1 HP1 HP1 HP1 SYNTHÈSE REVUES cellules de ces patients, une répression transcriptionnelle sur DUX4 est observée avec l'allongement expérimental des télomères [27]. Comme les symptômes de la myopathie FSH ne se déclarent pas avant 20 ou 30 ans, cette découverte a permis de proposer que le raccourcissement des télomères lié à l'âge pourrait être un élément déclencheur de la myopathie FSH chez des personnes présentant une contraction de la région 4q35.…”

Section: L'effet De Position Télomérique Chez L'hommeunclassified

“…Les données très récentes de Stadler et al [27] suggèrent néanmoins que, dans certaines conditions pathologiques de perturbation des subtélomères, comme dans la myopathie FSH, la répression transcriptionnelle dictée par le télomère puisse s'étendre sur plusieurs dizaines de kb en amont de celui-ci. Ceci souligne toute l'importance du bon fonctionnement des barrières subtélomériques naturelles contre la propagation de l'HC télomérique.…”

Section: Conclusion : Tpe or Not Tpe ?unclassified

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L’effet de position télomérique

Decottignies

2014

Med Sci (Paris)

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Facioscapulohumeral Muscular Dystrophy: Genetics

Magdinier

Upadhyaya

2018

Encyclopedia of Life Sciences

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Facioscapulohumeral muscular dystrophy (FSHD) is the third most common inherited muscular dystrophy that presents clinically with progressive weakness of the facial, scapular and humeral muscles, with later involvement of the trunk and lower extremities. FSHD is a unique disease with complex genetic and epigenetic aetiology and the underlying biological mechanisms are still not fully deciphered. FSHD1 is more frequent (95%) and is associated with the contraction of the D4Z4 macrosatellite repeat array located on a permissive 4qA chromosome combined with decreased methylation of cytosines at the 4q35‐linked D4Z4 units. D4Z4 contraction allows epigenetic derepression of the D4Z4 array allowing the expression of the toxic DUX4 transcription factor encoded within the terminal D4Z4 repeat in skeletal muscles. FSHD2 associated with approximately 2–3% of the FSHD patients results from haploinsufficiency of the SMCHD1 gene in individuals carrying a permissive 4qA allele and marked hypomethylation of 4q and 10q D4Z4, which leads to the derepression of DUX4 hence DUX4 appears to be a key player in both types of FSHD. Currently, there is no reliable treatment for this condition, therefore for the successful development of new treatments, an integration of clinical and pathogenetic information is vital. Key Concepts FSHD is the third most common inherited muscular dystrophy characterised by a typical phenotype and involvement of specific groups of muscles. FSHD is characterised by a highly variable penetrance and clinical severity. In most cases, FSHD involves shortening of a repetitive macrosatellite array. The D4Z4 macrosatellite linked to FSHD encodes the DUX4 transcription factor. A small proportion of FSHD patients carry mutation in the SMCHD1 gene. Epigenetic changes in FSHD are closely associated with molecular features. FSHD is a unique disease with complex genetic and epigenetic aetiology and the underlying biological mechanisms are still not fully deciphered. There is no reliable treatment for the disease.

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Telomere position effect regulates DUX4 in human facioscapulohumeral muscular dystrophy

Cited by 99 publications

References 48 publications

SORBS2transcription is activated by telomere position effect–over long distance upon telomere shortening in muscle cells from patients with facioscapulohumeral dystrophy

SORBS2transcription is activated by telomere position effect–over long distance upon telomere shortening in muscle cells from patients with facioscapulohumeral dystrophy

L’effet de position télomérique

Facioscapulohumeral Muscular Dystrophy: Genetics

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