[Complexity of the diagnosis of Wilson disease in clinical practice: our experience in 15 patients]

María Pilar Huarte-Muniesa; Esther Lacalle-Fabo; Juan Uriz-Otano; Silvia Berisa-Prado; Sira Moreno-Laguna; María Jesús Burusco-Paternáin

doi:10.1016/j.gastrohep.2014.02.007

[Complexity of the diagnosis of Wilson disease in clinical practice: our experience in 15 patients]

Gastroenterol Hepatol. 2014 Aug-Sep;37(7):389-96. doi: 10.1016/j.gastrohep.2014.02.007. Epub 2014 Apr 12.

[Article in Spanish]

Authors

María Pilar Huarte-Muniesa¹, Esther Lacalle-Fabo², Juan Uriz-Otano³, Silvia Berisa-Prado², Sira Moreno-Laguna⁴, María Jesús Burusco-Paternáin³

Affiliations

¹ Servicio de Aparato Digestivo, Complejo Hospitalario de Navarra, Pamplona, España. Electronic address: phuartem@cfnavarra.es.
² Servicio de Farmacia, Complejo Hospitalario de Navarra, Pamplona, España.
³ Servicio de Aparato Digestivo, Complejo Hospitalario de Navarra, Pamplona, España.
⁴ Servicio de Genética, Complejo Hospitalario de Navarra, Pamplona, España.

PMID: 24720933
DOI: 10.1016/j.gastrohep.2014.02.007

Abstract

Background: Wilson disease (WD) is an inherited disorder that causes copper (Cu) accumulation, leading to mainly liver, neurological and/or psychiatric manifestations. In the absence of some of the typical features, diagnosis of WD is difficult and is based on the combination of clinical, biochemical and genetic testing. The aim of this study was to illustrate the complexity of the approach to WD in daily clinical practice.

Methods: We retrospectively analyzed the medical records of patients with WD, including the clinical presentation, histological and biochemical findings, and follow up after treatment. We also carried out genetic testing, and the Leipzig diagnostic score was applied.

Results: We included 15 patients. Four were symptomatic, with liver (n=1), neurological (n=1), psychiatric (n=1) and mixed clinical manifestations (n=1), and 11 were presymptomatic, with elevated transaminases (n=8) and family study (n=3). We observed Kayser-Fleischer ring in 2 patients, both without neurologic symptoms. Ceruloplasmin ≤ 5 mg/dL was present in 73%, and 24-hour urinary Cu> 100 μg in 40%. Liver Cu was >250 μg/g.d.t. in 85% of the patients. The final diagnosis of WD was given by genetic testing (ATP7B gene mutations) in 5 patients with minimal disease features, including one symptomatic patient (psychiatric symptoms). We identified 5 previously reported mutations (p.M645R, p.R827W, p.H1069Q, p.P768L and p.G869R) and 3 unpublished mutations (p.L1313R, p.I1311T and p.A1179D); the most frequent mutation was p.M645R. After treatment, biochemical parameters (transaminases, urinary cooper) and symptoms improved, except in patients with neurological and psychiatric manifestations.

Conclusions: Our series illustrates the important role of genetic testing in the diagnosis of WD. The identification of the p.M645R mutation in most of our patients should be kept in mind in the molecular analysis of the ATP7B gene in our region.

Keywords: ATP7B gene; Enfermedad de Wilson; Estudio Genético; Gen ATP7B; Genetic testing; Leipzig score; Sales de Cinc; Score de Leipzig; Wilson Disease; Zinc salts.

Publication types

English Abstract

MeSH terms

Adolescent
Adult
Child
Diagnostic Tests, Routine
Female
Hepatolenticular Degeneration / diagnosis*
Hepatolenticular Degeneration / genetics
Humans
Male
Middle Aged
Retrospective Studies
Young Adult