Molecular Characterization of Wilson’s Disease in Liver Transplant Patients: A Five-Year Single-Center Experience in Iran
Zahra Beyzaei, Melika Majed, Seyed Mohsen Dehghani, Mohammad Hadi Imanieh, Ali Khazaee, Bita Geramizadeh, Ralf Weiskirchen

TL;DR
This study identifies new genetic mutations in Wilson’s disease among liver transplant patients in Iran, highlighting the importance of genetic testing in regions with high consanguinity.
Contribution
The study reports 21 previously unreported ATP7B mutations in Wilson’s disease patients from Iran, revealing population-specific genetic heterogeneity.
Findings
Twenty Wilson’s disease patients had 25 ATP7B variants, 21 of which were novel.
Most novel variants were damaging based on in silico analysis and affected key protein domains.
Consanguinity was common, with all compound-heterozygous cases arising from second-degree unions.
Abstract
Background/Objectives: Wilson’s disease (WD) is an autosomal recessive disorder characterized by pathological copper accumulation, primarily in the liver and brain. Severe hepatic involvement can be effectively treated with liver transplantation (LT). Geographic variation in ATP7B mutations suggests the presence of regional patterns that may impact disease presentation and management. This study aims to investigate the genetic basis of WD in patients from a major LT center in Iran. Methods: A retrospective analysis was conducted on clinical, biochemical, and pathological data from patients suspected of WD who underwent evaluation for LT between May 2020 and June 2025 at Shiraz University of Medical Sciences. Genetic testing was carried out on 20 patients at the Shiraz Transplant Research Center (STRC). Direct mutation analysis of ATP7B was performed for all patients, and the results…
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Taxonomy
TopicsTrace Elements in Health · Heavy Metal Exposure and Toxicity · Drug Transport and Resistance Mechanisms
