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Familial isolated hyperCKaemia associated with a new mutation in the caveolin-3 (CAV-3) gene
  1. L Merlini1,
  2. I Carbone5,
  3. C Capanni2,
  4. P Sabatelli3,
  5. S Tortorelli5,
  6. F Sotgia5,
  7. M P Lisanti4,
  8. C Bruno5,
  9. C Minetti5
  1. 1Neuromuscular Disease Unit, Istituto Ortopedico Rizzoli, Bologna, Italy
  2. 2Laboratory of Cellular Biology and Electron Microscopy, Istituto Ortopedico Rizzoli,
  3. 3Institute of Citomorphology, CNR, Bologna, Italy
  4. 4Department of Molecular Pharmacology, The Albert Einstein College of Medicine, Bronx, New York, USA
  5. 5Neuromuscular Disease Unit, Department of Paediatrics, University of Genova, Gaslini Institute, Genova, Italy
  1. Correspondence to:
 Dr C Minetti, Servizio Malattie Neuro-Muscolari, Dipartimento di Pediatria dell'Università di Genova, Istituto G Gaslini, Largo G Gaslini 5, I-16147 Genova, Italy;
 minettic{at}unige.it

Abstract

An 18 year old man and his mother both presented with persistent, isolated raised serum creatine kinase (hyperCKaemia) without muscle symptoms. Analysis of caveolin-3 protein expression in muscle biopsy of the propositus showed a reduction in the protein. Genetic analysis revealed a new heterozygous mutation in the caveolin-3 (CAV-3) gene: a C→T transition at nucleotide position 83 in exon 1 leading to a substitution of a proline for a leucine at amino acid position 28 (P28L). This is the first pathogenic mutation in the CAV-3 gene associated with isolated familial hyperCKaemia. It expands the genetic heterogeneity in patients with caveolin-3 deficiency and confirms that caveolin-3 deficiency should be considered in the differential diagnosis of isolated hyperCKaemia.

  • hyperCKaemia
  • caveolin-3
  • CAV-3 gene

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