Prognostic value of X-chromosome inactivation in symptomatic female carriers of dystrophinopathy

Author:

Juan-Mateu Jonàs,Rodríguez Maria José,Nascimento Andrés,Jiménez-Mallebrera Cecilia,González-Quereda Lidia,Rivas Eloy,Paradas Carmen,Madruga Marcos,Sánchez-Ayaso Pedro,Jou Cristina,González-Mera Laura,Munell Francina,Roig-Quilis Manuel,Rabasa Maria,Hernández-Lain Aurelio,Díaz-Manera Jorge,Gallardo Eduard,Pascual Jordi,Verdura Edgard,Colomer Jaume,Baiget Montserrat,Olivé Montse,Gallano Pia

Abstract

Abstract Background Between 8% and 22% of female carriers of DMD mutations exhibit clinical symptoms of variable severity. Development of symptoms in DMD mutation carriers without chromosomal rearrangements has been attributed to skewed X-chromosome inactivation (XCI) favouring predominant expression of the DMD mutant allele. However the prognostic use of XCI analysis is controversial. We aimed to evaluate the correlation between X-chromosome inactivation and development of clinical symptoms in a series of symptomatic female carriers of dystrophinopathy. Methods We reviewed the clinical, pathological and genetic features of twenty-four symptomatic carriers covering a wide spectrum of clinical phenotypes. DMD gene analysis was performed using MLPA and whole gene sequencing in blood DNA and muscle cDNA. Blood and muscle DNA was used for X-chromosome inactivation (XCI) analysis thought the AR methylation assay in symptomatic carriers and their female relatives, asymptomatic carriers as well as non-carrier females. Results Symptomatic carriers exhibited 49.2% more skewed XCI profiles than asymptomatic carriers. The extent of XCI skewing in blood tended to increase in line with the severity of muscle symptoms. Skewed XCI patterns were found in at least one first-degree female relative in 78.6% of symptomatic carrier families. No mutations altering XCI in the XIST gene promoter were found. Conclusions Skewed XCI is in many cases familial inherited. The extent of XCI skewing is related to phenotype severity. However, the assessment of XCI by means of the AR methylation assay has a poor prognostic value, probably because the methylation status of the AR gene in muscle may not reflect in all cases the methylation status of the DMD gene.

Publisher

Springer Science and Business Media LLC

Subject

Pharmacology (medical),Genetics(clinical),General Medicine

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