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The Wilson disease gene: spectrum of mutations and their consequences

Nature Genetics volume 9pages 210–217 (1995)Cite this article

A Correction to this article was published on 01 April 1995

Abstract

We have previously reported the cloning of a gene that encodes a copper transporting P–type ATPase (ATP7B) which is defective in Wilson disease. We have now identified in 58 WND patients, 20 new mutations as well as three of five previously published mutations: 11 small insertions and deletions, seven missense, two nonsense and three splice site mutations. Two of the mutations are relatively frequent, representing 38% of the mutations in patients of European origin. Our findings suggest a wider spectrum of age of onset than is considered typical of Wilson disease: mutations that completely disrupt the gene can produce liver disease in early childhood when Wilson disease may not typically considered in the differential diagnosis. The mutations identified provide an explanation for at least part of the wide phenotypic variation observed in Wilson disease.

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Authors and Affiliations

  1. Research Institute, The Hospital for Sick Children, Toronto, M5G 1X8, Canada

    Gordon R. Thomas, John R. Forbes, Eve A. Roberts & Diane W. Cox

  2. Department of Molecular and Medical Genetics, University of Toronto, Toronto, Canada

    Gordon R. Thomas, John R. Forbes & Diane W. Cox

  3. Department of Paediatrics, University of Toronto, Toronto, Canada

    Eve A. Roberts & Diane W. Cox

  4. Middlesex Hospital, London, UK

    John M. Walshe

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  1. Gordon R. Thomas
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  2. John R. Forbes
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  4. John M. Walshe
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  5. Diane W. Cox
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Thomas, G., Forbes, J., Roberts, E. et al. The Wilson disease gene: spectrum of mutations and their consequences. Nat Genet 9, 210–217 (1995). https://doi.org/10.1038/ng0295-210

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