Genetic and biochemical normalization in female carriers of Duchenne muscular dystrophy

Pegoraro, Elena; Schimke, R. Neil; García, Carmen; Stern, Harry A.; Cadaldini, Morena; Angelini, C.; Barbosa, Erika Ribeiro; Carroll, Judith; Marks, Warren A.; Neville, Hans E.; Marks, Harold G.; Appleton, Scott; Toriello, Helga V.; Wessel, Henry B.; Donnelly, J. E.; Bernes, Saunder; Taber, Joseph W.; Weiss, Lee E.; Hoffman, Eric P.

doi:10.1212/wnl.45.4.677

Cited by 89 publications

(57 citation statements)

References 18 publications

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“…40 It is estimated that, in order to effect a cure of dystrophic muscle using a gene therapy approach, between 20 and 50% of muscle fibres of all affected muscles must express dystrophin. 41 Our data on mdx in this paper is consistent with this conclusion. Currently replacement of up to 50% of skeletal muscle dystrophin in DMD patients is a technically insurmountable feat.…”

Section: Possible Therapeutic Approaches For Dmdsupporting

confidence: 89%

IGF-II ameliorates the dystrophic phenotype and coordinately down-regulates programmed cell death

et al. 2000

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Duchenne muscular dystrophy (DMD) is a fatal and crippling disease of skeletal muscle which displays increased fibre turnover and elevated levels of programmed cell death (PCD) in muscle stem cells. Previously we showed that this cell death is inhibited by the growth factor IGF-II. To determine the functional significance of PCD to the dystrophic phenotype, we used a transgene to over-express IGF-II in the mdx mouse. We found that ectopic expression of IGF-II inhibited the elevated PCD observed in skeletal muscles in the absence of functional dystrophin and significantly ameliorates the early gross histopathological changes in skeletal muscles characteristic of the dystrophic phenotype. Replacement of the dystrophin gene abolished abnormal skeletal muscle cell PCD levels in vivo in a dose-dependent manner and in dystrophic SMS cell lines cultured in vitro. Thus elevation of stem cell PCD in dystrophic skeletal muscle is a direct consequence of the loss of functional dystrophin. Together these data demonstrate that elevated skeletal muscle cell PCD is a critical component of dystrophic pathology and is inversely correlated with both dystrophin gene dosage and with muscle fibre pathology. Targeting PCD in dystrophic muscles reduces both PCD and the classical features of dystrophic pathology in the mdx mouse suggesting that IGF-II is a strong candidate for therapeutic intervention in the dystrophinopathies.

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Section: Possible Therapeutic Approaches For Dmdsupporting

confidence: 89%

IGF-II ameliorates the dystrophic phenotype and coordinately down-regulates programmed cell death

et al. 2000

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“…Furthermore, XCI pattern may be modified in multinucleate muscle fibers compared with single nucleate lymphocytes. 37 Indeed, Pegoraro et al 37 proposed a model of biochemical normalization in random inactivation patients and genetic normalization in skewed X-inactivation carriers. This could explain the preferential normal expressed allele in patient #25 explored at 46 years, but this model cannot be applied to the 38% of manifesting carriers with random XCI in our cohort.…”

Section: Muscle Study and Protein Expression In The Musclementioning

confidence: 99%

Genetic and clinical specificity of 26 symptomatic carriers for dystrophinopathies at pediatric age

et al. 2013

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The molecular basis underlying the clinical variability in symptomatic Duchenne muscular dystrophy (DMD) carriers are still to be precised. We report 26 cases of early symptomatic DMD carriers followed in the French neuromuscular network. Clinical presentation, muscular histological analysis and type of gene mutation, as well as X-chromosome inactivation (XCI) patterns using DNA extracted from peripheral blood or muscle are detailed. The initial symptoms were significant weakness (88%) or exercise intolerance (27%). Clinical severity varied from a Duchenne-like progression to a very mild Becker-like phenotype. Cardiac dysfunction was present in 19% of the cases. Cognitive impairment was worthy of notice, as 27% of the carriers are concerned. The muscular analysis was always contributive, revealing muscular dystrophy (83%), mosaic in immunostaining (81%) and dystrophin abnormalities in western blot analysis (84%). In all, 73% had exonic deletions or duplications and 27% had point mutations. XCI pattern was biased in 62% of the cases. In conclusion, we report the largest series of manifesting DMD carriers at pediatric age and show that exercise intolerance and cognitive impairment may reveal symptomatic DMD carriers. The complete histological and immunohistological study of the muscle is the key of the diagnosis leading to the dystrophin gene analysis. Our study shows also that cognitive impairment in symptomatic DMD carriers is associated with mutations in the distal part of the DMD gene. XCI study does not fully explain the mechanisms as well as the wide spectrum of clinical phenotype, though a clear correlation between the severity of the phenotype and inactivation bias was observed. European Journal of Human Genetics (2013) 21, 855-863; doi:10.1038/ejhg.2012.269; published online 9 January 2013 Keywords: dystrophin; female carrier; X inactivation INTRODUCTION Duchenne muscular dystrophy (DMD) has always been extensively described in its clinical presentation, evolution and severity. 1 However, recent studies pointed out that the same mutation can be responsible for DMD phenotypes of different severity suggesting involvement of modifier and/or epigenetic factors. 2,3 It has been estimated that about 8% of DMD female carriers have some manifestations including cardiomyopathy and/or some degree of weakness that could be highlighted by careful clinical examination. [4][5][6][7][8] Relationships between clinical phenotype and dystrophin abnormalities in muscle tissue among female carriers of DMD gene mutations were previously investigated. 9 However, a comprehensive view of factors underlying clinical symptoms occurrence and severity is still lacking.

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“…It has been shown previously that dystrophin-expressing muscle fibers have a biochemical advantage for survival over dystrophin-deficient muscle fibers. 17 Therefore, future studies are warranted to explore the long-term therapeutic effects of dystrophin gene delivery in utero using HC-Ad vectors.…”

Section: Discussionmentioning

confidence: 99%

Comparison of high-capacity and first-generation adenoviral vector gene delivery to murine muscle in utero

Bilbao

Reay

et al. 2004

Gene Ther

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Genetic and biochemical normalization in female carriers of Duchenne muscular dystrophy

Cited by 89 publications

References 18 publications

IGF-II ameliorates the dystrophic phenotype and coordinately down-regulates programmed cell death

IGF-II ameliorates the dystrophic phenotype and coordinately down-regulates programmed cell death

Genetic and clinical specificity of 26 symptomatic carriers for dystrophinopathies at pediatric age

Comparison of high-capacity and first-generation adenoviral vector gene delivery to murine muscle in utero

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