Arch Med Res. 2026 Mar 16;57(5):103407. doi: 10.1016/j.arcmed.2026.103407. Online ahead of print.
ABSTRACT
BACKGROUND: Wilson disease (WD) is a multisystemic disorder caused by a disturbance in copper homeostasis due to pathogenic biallelic variants in the ATP7B gene.
AIM: To identify the pathogenic variants in the ATP7B gene in Mexican individuals with WD and describe their phenotypic presentation.
METHODS: We included 19 individuals from 11 unrelated families with molecularly confirmed WD.
RESULTS: 52.6% of the WD patients were male, and three were asymptomatic at diagnosis. The median age at presentation was 19 years. Of the symptomatic individuals, 84.2% had hepatic manifestations, 62.5% had neurological symptoms, 25.0% had psychiatric manifestations, and 90.9% had Kayser-Fleischer rings. The phenotypic distribution was as follows: combined (52.6%), acute liver failure (26.3%), chronic liver disease (5.3%), and asymptomatic (15.8%). Modified Leipzig scores ranged from 8 to 16. Five patients underwent liver transplantation, and eight patients were treated with copper chelators. Eight different pathogenic variants were identified, including the recurrent c.3207C>A and c.3809A>G, as described in other series.
CONCLUSIONS: We present the first and largest case series of Mexican patients with WD confirmed by molecular testing. All patients exhibited hepatic manifestations. The most frequent phenotypes were combined (52.6%) and acute liver failure (26.3%). A statistically significant difference in the frequency of asymptomatic patients was observed between the homozygous c.3207C>A genotype group and the group with other genotypes (p = 0.036). The modified Leipzig score is a valuable diagnostic tool for WD.
PMID:41844444 | DOI:10.1016/j.arcmed.2026.103407
