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September 23, 2003; 61 (6) Brief Communications

Rapsyn mutations in hereditary myasthenia

Distinct early- and late-onset phenotypes

G. Burke, J. Cossins, S. Maxwell, G. Owens, A. Vincent, S. Robb, M. Nicolle, D. Hilton–Jones, J. Newsom–Davis, J. Palace, D. Beeson
First published September 22, 2003, DOI: https://doi.org/10.1212/01.WNL.0000085865.55513.AE
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Abstract

Rapsyn mutations in 16 unrelated patients with a congenital/hereditary myasthenic syndrome were identified, and a mutation (N88K) common to each of them was found. Two distinct phenotypes were noted: early and late onset. The former is frequently associated with arthrogryposis multiplex congenita and life-threatening crises. The late-onset phenotype developed in adolescence or adulthood and was initially mistaken for seronegative myasthenia gravis. Recognition of this late-onset phenotype should prevent inappropriate immunotherapy.

  • Received February 10, 2003.
  • Accepted May 20, 2003.
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