Skip to main page content
U.S. flag

An official website of the United States government

Dot gov

The .gov means it’s official.
Federal government websites often end in .gov or .mil. Before sharing sensitive information, make sure you’re on a federal government site.

Https

The site is secure.
The https:// ensures that you are connecting to the official website and that any information you provide is encrypted and transmitted securely.

Access keys NCBI Homepage MyNCBI Homepage Main Content Main Navigation
. 2017 Nov 14;18(Suppl 8):819.
doi: 10.1186/s12864-017-4188-2.

Genotypic and phenotypic features of all Spanish patients with McArdle disease: a 2016 update

Alfredo Santalla  1   2 Gisela Nogales-Gadea  3   4 Alberto Blázquez Encinar  2   5   6 Irene Vieitez  7 Adrian González-Quintana  2   5 Pablo Serrano-Lorenzo  2   5 Inés García Consuegra  2   5   6 Sara Asensio  2   5 Alfonsina Ballester-Lopez  8   5 Guillem Pintos-Morell  8   9   5 Jaume Coll-Cantí  8   5   10 Helios Pareja-Galeano  2   11 Jorge Díez-Bermejo  2   11 Margarita Pérez  11 Antoni L Andreu  12 Tomàs Pinós  5   12 Joaquín Arenas  2   5 Miguel A Martín  2   5   6 Alejandro Lucia  2   11
Affiliations

Genotypic and phenotypic features of all Spanish patients with McArdle disease: a 2016 update

Alfredo Santalla et al. BMC Genomics. .

Abstract

Background: We recently described the genotype/phenotype features of all Spanish patients diagnosed with McArdle disease as of January 2011 (n = 239, prevalence of ~1/167,000) (J Neurol Neurosurg Psychiatry 2012;83:322-8). Several caveats were however identified suggesting that the prevalence of the disease is actually higher.

Methods: We have now updated main genotype/phenotype data, as well as potential associations within/between them, of all Spanish individuals currently diagnosed with McArdle disease (December 2016).

Results: Ninety-four new patients (all Caucasian) have been diagnosed, yielding a prevalence of ~1/139,543 individuals. Around 55% of the mutated alleles have the commonest PYGM pathogenic mutation p.R50X, whereas p.W798R and p.G205S account for 10 and 9% of the allelic variants, respectively. Seven new mutations were identified: p.H35R, p.R70C, p.R94Q, p.L132WfsX163, p.Q176P, p.R576Q, and c.244-3_244-2CA. Almost all patients show exercise intolerance, the second wind phenomenon and high serum creatine kinase activity. There is, however, heterogeneity in clinical severity, with 8% of patients being asymptomatic during normal daily life, and 21% showing limitations during daily activities and fixed muscle weakness. A major remaining challenge is one of diagnosis, which is often delayed until the third decade of life in 72% of new patients despite the vast majority (86%) reporting symptoms before 20 years. An important development is the growing proportion of those reporting a 4-year improvement in disease severity (now 34%) and following an active lifestyle (50%). Physically active patients are more likely to report an improvement after a 4-year period in the clinical course of the disease than their inactive peers (odds ratio: 13.98; 95% confidence interval: 5.6, 34.9; p < 0.001). Peak oxygen uptake is also higher in the former (20.7 ± 6.0 vs. 16.8 ± 5.3 mL/kg/min, p = 0.0013). Finally, there is no association between PYGM genotype and phenotype manifestation of the disease.

Conclusions: The reported prevalence of McArdle disease grows exponentially despite frequent, long delays in genetic diagnosis, suggesting that many patients remain undiagnosed. Until a genetic cure is available (which is not predicted in the near future), current epidemiologic data support that adoption of an active lifestyle is the best medicine for these patients.

Keywords: Genotype; Glycogenosis type V; McArdle disease; Phenotype; Spanish patients.

PubMed Disclaimer

Conflict of interest statement

Ethics approval and consent to participate

All participants were informed of the purposes of that project and signed a written consent. This study was approved by the local institutional ethics committees (CEIC i + 12 14/357, PT13/0010/0022) and was in accordance with the Declaration of Helsinki for Human Research.

Consent for publication

Not applicable.

Competing interests

The authors declare that they have no competing interests.

Publisher’s Note

Springer Nature remains neutral with regard to jurisdictional claims in published maps and institutional affiliations.

References

    1. Lucia A, Nogales-Gadea G, Perez M, Martin MA, Andreu AL, Arenas J. McArdle disease: what do neurologists need to know? Nat Clin Pract Neurol. 2008;4(10):568–577. doi: 10.1038/ncpneuro0913. - DOI - PubMed
    1. Vissing J, Haller RG. A diagnostic cycle test for McArdle's disease. Ann Neurol. 2003;54(4):539–542. doi: 10.1002/ana.10725. - DOI - PubMed
    1. Bruno C, Cassandrini D, Martinuzzi A, Toscano A, Moggio M, Morandi L, Servidei S, Mongini T, Angelini C, Musumeci O, et al. McArdle disease: the mutation spectrum of PYGM in a large Italian cohort. Hum Mutat. 2006;27(7):718. doi: 10.1002/humu.9434. - DOI - PubMed
    1. Martin MA, Rubio JC, Buchbinder J, Fernandez-Hojas R, del Hoyo P, Teijeira S, Gamez J, Navarro C, Fernandez JM, Cabello A, et al. Molecular heterogeneity of myophosphorylase deficiency (McArdle's disease): a genotype-phenotype correlation study. Ann Neurol. 2001;50(5):574–581. doi: 10.1002/ana.1225. - DOI - PubMed
    1. Martinuzzi A, Sartori E, Fanin M, Nascimbeni A, Valente L, Angelini C, Siciliano G, Mongini T, Tonin P, Tomelleri G, et al. Phenotype modulators in myophosphorylase deficiency. Ann Neurol. 2003;53(4):497–502. doi: 10.1002/ana.10499. - DOI - PubMed

LinkOut - more resources