In-Frame Deletion of Dystrophin Exons 8–50 Results in DMD Phenotype

Егорова, Т. В.; Galkin, Ivan I.; Velyaev, Oleg A.; Vassilieva, Svetlana G.; Savchenko, Irina M.; Loginov, V.; Dzhenkova, Marina A.; Korshunova, Diana S.; Козлова, О. С.; Ivankov, Dmitry N.; Polikarpova, Anna V.

doi:10.3390/ijms24119117

Cited by 4 publications

(1 citation statement)

References 60 publications

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“…The cysteine-rich domain consists of subdomains WW (tryptophan-rich domain), EFH1, EFH2 (EF hand domains 1 and 2), and ZZ (zinc finger domain) ( 18 ).…”

Section: Literature Search and Clinical Categorizationmentioning

confidence: 99%

DMD deletions underlining mild dystrophinopathies: literature review highlights phenotype-related mutation clusters and provides insights about genetic mechanisms and prognosis

Fortunato,

Tonelli,

Farnè

et al. 2024

Front. Neurol.

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DMD gene pathogenic variations cause a spectrum of phenotypes, ranging from severe Duchenne muscular dystrophy, the Becker milder cases, the intermediate or very mild muscle phenotypes invariably characterized by high CK, and the ultrarare fully-asymptomatic cases. Besides these phenotypes, X-linked dilated cardiomyopathy is also caused by DMD mutations. Males carrying DMD deletions with absent or very mild phenotypes have been sparsely described. We performed a horizon scan on public datasets to enroll males with the above phenotypes and carrying DMD deletions to delineate myopathic genotype-phenotype relationships. We inventoried 81 males, who were divided into the following clinical categorization: fully-asymptomatic males aged >43 years (A, N = 22); isolated hyperCKemia (CK, N = 35); and mild weakness (any age) with or without high CK (WCK, N = 24). In all cases, deleted intervals were exons 2 to 55, and no downstream exons were ever involved, apart from an exon 78 deletion in a WCK patient. All deletions were in-frame apart from the known exception to the rule of exon 2 and exon 78. We correlated the mild phenotypes (A and CK) to deleted exons, intronic breakpoints, exon-exon junctions, 3′ isoforms rule, and protein epitopes, and we found that some genetic profiles are exclusively/mainly occurring in A/CK phenotypes, suggesting they are compatible with a quasi-normal muscular performance. We discussed diverse pathogenic mechanisms that may contribute to mild dystrophinopathic phenotypes, and we tried to address some “critical” genetic configurations or exon content needed to preserve a semi-functional DMD gene.

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“…The cysteine-rich domain consists of subdomains WW (tryptophan-rich domain), EFH1, EFH2 (EF hand domains 1 and 2), and ZZ (zinc finger domain) ( 18 ).…”

Section: Literature Search and Clinical Categorizationmentioning

confidence: 99%