Next-generation sequencing approach to hyperCKemia

Rubegni, Anna; Malandrini, Alessandro; Dosi, Claudia; Astrea, Guja; Baldacci, Jacopo; Battisti, Carla; Bertocci, Giulia; Dotti, Maria Teresa; Federico, Antonio; Giannini, Francesco; Grosso, Salvatore; Guerrini, Renzo; Lenzi, Sara; Maioli, Maria Antonietta; Melani, Federico; Sacchini, Michele; Salvatore, Simona; Siciliano, Gabriele; Tolomeo, Deborah; Tonin, Paola; Volpi, Nila; Santorelli, Filippo M.; Cassandrini, Denise

doi:10.1212/nxg.0000000000000352

Cited by 31 publications

(37 citation statements)

References 48 publications

(32 reference statements)

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“…In addition, we describe exertional rhabdomyolysis in two siblings (3/III.1 and 3/III.2 in Figure 1). Although this clinical presentation has to be confirmed for other reported cases before considering it a definite feature of calpainopathies, such a presentation has already been described for other genes associated with LGMD, such as CAV3 , GMPPB and more recently SGCA and TCAP [34‐36]. Thus, autosomal dominant inherited calpainopathy should be considered when faced by a wide range of initial phenotypic presentations from hyperCKaemia (asymptomatic or not), myalgia with or without exertional rhabdomyolysis to mild LGMD.…”

Section: Discussionmentioning

confidence: 60%

Novel CAPN3 variant associated with an autosomal dominant calpainopathy

Cerino

Campana‐Salort

Salvi

et al. 2020

Neuropathology Appl Neurobio

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Section: Discussionmentioning

confidence: 60%

Novel CAPN3 variant associated with an autosomal dominant calpainopathy

Cerino

Campana‐Salort

Salvi

et al. 2020

Neuropathology Appl Neurobio

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“…[102][103][104] In addition to those with overt clinical, electrodiagnostic (EDx), or histological evidence of a myopathy, genetic testing can also be considered in certain patients with asymptomatic CK elevations. 105,106 Even in these asymptomatic patients, genetic testing can alter management, for example, by detecting dystrophinopathy carrier status or RYR1 mutations predisposing to malignant hyperthermia. 105,106 Genetic testing previously centered around serial sequencing of single genes, with the testing sequence guided by patients' phenotypes, histological findings and suspected mode of inheritance.…”

Section: General Approachmentioning

confidence: 99%

Guidelines for genetic testing of muscle and neuromuscular junction disorders

2021

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Despite recent advances in the understanding of inherited muscle and neuromuscular junction diseases, as well as the advent of a wide range of genetic tests, patients continue to face delays in diagnosis of sometimes treatable disorders. These guidelines outline an approach to genetic testing in such disorders. Initially, a patient's phenotype is evaluated to identify myopathies requiring directed testing, including myotonic dystrophies, facioscapulohumeral muscular dystrophy, oculopharyngeal muscular dystrophy, mitochondrial myopathies, dystrophinopathies, and oculopharyngodistal myopathy. Initial investigation in the remaining patients is generally a comprehensive gene panel by next-generation sequencing. Broad panels have a higher diagnostic yield and can be cost-effective. Due to extensive phenotypic overlap and treatment implications, genes responsible for congenital myasthenic syndromes should be included when evaluating myopathy patients. For patients whose initial genetic testing is negative or inconclusive, phenotypic re-evaluation is warranted, along with consideration of genes and variants not included initially, as well as their acquired mimickers.

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“…Il percorso nel paziente pediatrico, in caso di valori moderati-alti e persistenti di CPK (>1000 U/L), prosegue in genere con l'analisi enzimatica e molecolare (esistono pannelli disponibili) e, meno frequentemente rispetto all'adulto, con l'elettromiografia e la biopsia muscolare. Lo spettro delle miopatie è tuttavia molto ampio e non ancora pienamente conosciuto, rendendo pertanto necessario nella maggior parte dei casi l'invio del bambino a un centro di riferimento per patologie neuromuscolari [1,3]. Tra le cause di miopatia metabolica, la malattia di Pompe è una patologia rara (incidenza della forma adulta di 1:60.000 nella popolazione europea), ma probabilmente sottostimata.…”

Section: Commentounclassified

Dal fegato al muscolo: una rara malattia a esordio tardivo

Brusadelli

Calia

Fasoli³

et al. 2021

QACP

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We describe the case of a seven-year-old child who, following the incidental finding of hypertransaminasemia in the blood tests performed for a lymphadenopathy, is subjected to other blood tests that show a persistent moderate increase in CPK values, supporting the hypothesis of a muscle disease even in the absence of specific symptoms. The diagnostic path seems to point towards a late-onset metabolic myopathy. The occasional finding of hypertransaminases , associated with the finding of high CPK levels in an asymptomatic or paucisymptomatic child, orients the diagnostic path. Excluding hepatic storage disease or viral infectious disease, the differential diagnosis leads to a complex late-onset myopathy such as Pompe disease, a rare but important diagnosis whose prognosis could be dramatically improved by the enzyme replacement therapy.

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Next-generation sequencing approach to hyperCKemia

Cited by 31 publications

References 48 publications

Novel CAPN3 variant associated with an autosomal dominant calpainopathy

Novel CAPN3 variant associated with an autosomal dominant calpainopathy

Guidelines for genetic testing of muscle and neuromuscular junction disorders

Dal fegato al muscolo: una rara malattia a esordio tardivo

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