| Literature DB >> 33573009 |
Cigdem Yuce Kahraman1, Ali Islek2, Abdulgani Tatar1, Özlem Özdemir3, Adil Mardinglu4,5, Hasan Turkez6.
Abstract
Wilson disease (WD) (OMIM# 277900) is an autosomal recessive inherited disorder characterized by excess copper (Cu) storage in different human tissues, such as the brain, liver, and the corneas of the eyes. It is a rare disorder that occurs in approximately 1 in 30,000 individuals. The clinical presentations of WD are highly varied, primarily consisting of hepatic and neurological conditions. WD is caused by homozygous or compound heterozygous mutations in the ATP7B gene. The diagnosis of the disease is complicated because of its heterogeneous phenotypes. The molecular genetic analysis encourages early diagnosis, treatment, and the opportunity to screen individuals at risk in the family. In this paper, we reported a case with a novel, hotspot-located mutation in WD. We have suggested that this mutation in the ATP7B gene might contribute to liver findings, progressing to liver failure with a loss of function effect. Besides this, if patients have liver symptoms in childhood and/or are children of consanguineous parents, WD should be considered during the evaluation of the patients.Entities:
Keywords: ATP7B; Wilson disease; copper; liver failure; novel mutation; rare disorder
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Year: 2021 PMID: 33573009 PMCID: PMC7912016 DOI: 10.3390/medicina57020123
Source DB: PubMed Journal: Medicina (Kaunas) ISSN: 1010-660X Impact factor: 2.430