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Bethlem myopathy: a series of 16 patients and description of seven new associated mutations

  • Luísa Panadés-de OliveiraEmail author
  • Claudia Rodríguez-López
  • Diana Cantero Montenegro
  • María del Mar Marcos Toledano
  • Ana Fernández-Marmiesse
  • Jesús Esteban Pérez
  • Aurelio Hernández Lain
  • Cristina Domínguez-González
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Abstract

Background

Bethlem myopathy represents the milder phenotype of collagen type VI-related myopathies. However, clinical manifestations are highly variable among patients and no phenotype-genotype correlation has been described. We aim to analyse the clinical, pathological and genetic features of a series of patients with Bethlem myopathy, and we describe seven new mutations.

Methods

A series of 16 patients with the diagnosis of Bethlem myopathy were analyzed retrospectively from their medical records for clinical, creatine kinase (CK), muscle biopsy, and muscle magnetic resonance (MRI) data. Genetic testing was performed through next-generation sequencing of custom amplicon-based targeted genes panel of myopathies. Mutations were confirmed by Sanger sequencing.

Results

The most frequent phenotype consisted of proximal limb weakness associated with interphalangeal and wrists contractures. However, cases with isolated contractures or isolated myopathy were found. CK levels did not correlate with severity of the disease. The most frequent mutation was the COL6A3 variant c.7447A>G, p.Lys2486Glu, with either an homozygous or compound heterozygous presentation. Five new mutations were found in COL6A1 gene and other two in COL6A3 gene, all of them with a dominant heritability pattern. From these, a new COL6A1 mutation (c.1657G>A, p.Glu553Arg) was related to an oligosymptomatic phenotype with predominating contractures in the absence of weakness and a normal muscle MRI. Finally, the most common COL6A1 mutation reported to date that leads to an Ullrich phenotype (c. 868G>A, p.Gly290Arg), has been found here as Bethlem presentation.

Conclusions

Manifestations of Bethlem myopathy are quite variable, so either contractures or weakness may be lacking, and no phenotype-genotype associations can be brought.

Keywords

Bethlem myopathy Joint contractures Proximal muscular weakness COL6 genes Collagen type VI-related myopathies 
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Notes

Funding

There is no funding.

Compliance with ethical standards

Conflicts of interest

The authors declare that they have no competing interests.

References

  1. 1.
    Briñas L, Richard P, Quijano-Roy S, Gartioux C, Ledeuil C, Lacène E et al (2010) Early onset collagen VI myopathies: genetic and clinical correlations. Ann Neurol 68(4):511–520CrossRefGoogle Scholar
  2. 2.
    Merlini L, Martoni E, Grumati P, Sabatelli P, Squarzoni S, Urciuolo A et al (2008) Autosomal recessive myosclerosis myopathy is a collagen VI disorder. Neurology 71(16):1245–1253CrossRefGoogle Scholar
  3. 3.
    Scacheri PC, Gillanders EM, Subramony SH, Vedanarayanan V, Crowe CA, Thakore N et al (2002) Novel mutations in collagen VI genes: expansion of the Bethlem myopathy phenotype. Neurology 58(4):593–602CrossRefGoogle Scholar
  4. 4.
    Okada M, Kawahara G, Noguchi S, Sugie K, Murayama K, Nonaka I et al (2007) Primary collagen VI deficiency is the second most common congenital muscular dystrophy in Japan. Neurology 69(10):1035–1042CrossRefGoogle Scholar
  5. 5.
    Kim SY, Kim WJ, Kim H, Choi SA, Lee JS, Cho A et al (2018) Collagen VI-related myopathy: expanding the clinical and genetic spectrum. Muscle Nerve 58(3):381–388CrossRefGoogle Scholar
  6. 6.
    Foley AR, Hu Y, Zou Y, Columbus A, Shoffner J, Dunn DM et al (2009) Autosomal recessive inheritance of classic Bethlem myopathy. Neuromuscul Disord 19(12):813–817CrossRefGoogle Scholar
  7. 7.
    Gualandi F, Urciuolo A, Martoni E, Sabatelli P, Squarzoni S, Bovolenta M et al (2009) Autosomal recessive Bethlem myopathy. Neurology 73(22):1883–1891CrossRefGoogle Scholar
  8. 8.
    González-Pérez A, López-Bigas N (2011) Improving the assessment of the outcome of nonsynonymous SNVs with a consensus deleteriousness score, Condel. Am J Hum Genet 88(4):440–449CrossRefGoogle Scholar
  9. 9.
    Desmet F-O, Hamroun D, Lalande M, Collod-Béroud G, Claustres M, Béroud C (2009) Human splicing finder: an online bioinformatics tool to predict splicing signals. Nucleic Acids Res 37(9):e67–e67CrossRefGoogle Scholar
  10. 10.
    Mercuri E, Lampe A, Allsop J, Knight R, Pane M, Kinali M et al (2005) Muscle MRI in Ullrich congenital muscular dystrophy and Bethlem myopathy. Neuromuscul Disord 15(4):303–310CrossRefGoogle Scholar
  11. 11.
    Fu J, Zheng Y-M, Jin S-Q, Yi J-F, Liu X-J, Lyn H et al (2016) “Target” and “Sandwich” signs in thigh muscles have high diagnostic values for collagen VI-related myopathies. Chin Med J 129(15):1811CrossRefGoogle Scholar
  12. 12.
    Lampe AK, Dunn DM, von Niederhausern AC, Hamil C, Aoyagi A, Laval SH et al (2005) Automated genomic sequence analysis of the three collagen VI genes: applications to Ullrich congenital muscular dystrophy and Bethlem myopathy. J Med Genet 42(2):108–120CrossRefGoogle Scholar
  13. 13.
    Hunter JM, Ahearn ME, Balak CD, Liang WS, Kurdoglu A, Corneveaux JJ et al (2015) Novel pathogenic variants and genes for myopathies identified by whole exome sequencing. Mol Genet Genom Med 3(4):283–301CrossRefGoogle Scholar
  14. 14.
    Martins AI, Maarque C, Pinto-Basto K, Negrão L (2017) Bethlem myopathy in a Portuguese patient—case report. Acta Myol 36(3):178–181Google Scholar
  15. 15.
    Fan Y, Liu A, Wei C, Yang H, Chang X, Wang S et al (2018) Genetic and clinical findings in a Chinese cohort of patients with collagen VI-related myopathies. Clin Genet 93(6):1159–1171CrossRefGoogle Scholar
  16. 16.
    Suárez B, Lozano-Arango A, Araneda D, Cortés F, Hervias C, Calcagno G et al (2018) Collagen VI related myopathies. When to suspect, how to identify. The contribution of muscle magnetic resonance. Rev Chil Pediatr 89(3):399–408Google Scholar
  17. 17.
    Butterfield RJ, Foley AR, Dastgir J, Asman S, Dunn DM, Zou Y et al (2013) Position of glycine substitutions in the triple helix of COL6A1, COL6A2, and COL6A3 is correlated with severity and mode of inheritance in collagen VI myopathies. Hum Mutat 34(11):1558–1567CrossRefGoogle Scholar
  18. 18.
    Pace RA, Peat RA, Baker NL, Zamurs L, Mörgelin M, Irving M et al (2008) Collagen VI glycine mutations: perturbed assembly and a spectrum of clinical severity: collagen VI glycine mutations. Ann Neurol 64(3):294–303CrossRefGoogle Scholar
  19. 19.
    Reddy HM, Cho K-A, Lek M, Estrella E, Valkanas E, Jones MD et al (2017) The sensitivity of exome sequencing in identifying pathogenic mutations for LGMD in the United States. J Hum Genet 62(2):243–252CrossRefGoogle Scholar
  20. 20.
    Giusti B, Lucarini L, Pietroni V, Lucioli S, Bandinelli B, Sabatelli P et al (2005) Dominant and recessive COL6A1 mutations in Ullrich scleroatonic muscular dystrophy. Ann Neurol 58(3):400–410CrossRefGoogle Scholar
  21. 21.
    Deconinck N, Richard P, Allamand V, Behin A, Laforet P, Ferreiro A et al (2015) Bethlem myopathy: long-term follow-up identifies COL6 mutations predicting severe clinical evolution. J Neurol Neurosurg Psychiatry 86(12):1337–1346Google Scholar

Copyright information

© Springer-Verlag GmbH Germany, part of Springer Nature 2019

Authors and Affiliations

  • Luísa Panadés-de Oliveira
    • 1
    Email author
  • Claudia Rodríguez-López
    • 1
  • Diana Cantero Montenegro
    • 2
  • María del Mar Marcos Toledano
    • 3
  • Ana Fernández-Marmiesse
    • 4
  • Jesús Esteban Pérez
    • 1
    • 5
  • Aurelio Hernández Lain
    • 2
  • Cristina Domínguez-González
    • 1
    • 5
    • 6
    • 7
  1. 1.Department of NeurologyHospital Universitario 12 de OctubreMadridSpain
  2. 2.Department of NeuropathologyHospital Universitario 12 de OctubreMadridSpain
  3. 3.Department of NeurologyHospital Universitario de BadajozBadajozSpain
  4. 4.Centro de Investigación en Enfermedades Crónicas (CIMUS)-Grupo de Genomas y Enfermedad P2L9Universidad de Santiago de CompostelaSantiago de CompostelaSpain
  5. 5.Neuromuscular Disorders Unit, Department of NeurologyHospital Universitario 12 de OctubreMadridSpain
  6. 6.Centro de Investigación Biomédica en Red de Enfermedades Raras (CIBERER), U723MadridSpain
  7. 7.Instituto de investigación i+12MadridSpain

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