Clinical Research
Copyright ©The Author(s) 2004. Published by Baishideng Publishing Group Inc. All rights reserved.
World J Gastroenterol. Feb 15, 2004; 10(4): 590-593
Published online Feb 15, 2004. doi: 10.3748/wjg.v10.i4.590
Correlation of ATP7B genotype with phenotype in Chinese patients with Wilson disease
Xiao-Qing Liu, Ya-Fen Zhang, Tze-Tze Liu, Kwang-Jen Hsiao, Jian-Ming Zhang, Xue-Fan Gu, Ke-Rong Bao, Li-Hua Yu, Mei-Xian Wang
Xiao-Qing Liu, Jian-Ming Zhang, Ke-Rong Bao, Li-Hua Yu, Mei-Xian Wang, Department of Neurology, Xinhua Hospital, Shanghai Second Medical University, Shanghai 200092, China
Ya-Fen Zhang, Xue-Fan Gu, Shanghai Institute for Pediatric Research, Shanghai 200092, China
Tze-Tze Liu, Kwang-Jen Hsiao, Genome Research Center and Institute of Genetics, National Yang Ming University, and Department of Medical Research and Education, Taipei Veterans General Hospital, Taipei 11216, Taiwan, China
Author contributions: All authors contributed equally to the work.
Supported by the National Ministry of Education Teacher Education Plan in China 2000 NO.1424
Correspondence to: Dr. Xiao-Qing Liu, Department of Neurology, Xinhua Hospital, Shanghai Second Medical University, 1665 Kongjiang Rd, Shanghai 200092, China. xqliu@public8.sta.net.cn
Telephone: +86-21-65790000 Fax: +86-21-65791316
Received: June 30, 2003
Revised: July 14, 2003
Accepted: July 30, 2003
Published online: February 15, 2004
Abstract

AIM: To determine the mutational characterization of P-type ATP7B gene and to explore the correlation of ATP7B genotype to phenotype in Chinese patients with Wilson disease (WD).

METHODS: Seventy-five patients with WD from 72 no-kinship families, 44 males and 31 females, were enrolled in this study. The age of onset ranged from 4 to 39 years, ≤ 18 years in 72 patients. Some exons of ATP7B gene mutations were analyzed in patients with WD by using biochemical methods, polymerase chain reaction-single strand configuration polymorphism (PCR-SSCP) and DNA sequence analysis. A total of 778 coding regions were identified with restriction enzyme Msp I. The activity of Cu-ATPase was assessed by measuring inorganic phosphorus.

RESULTS: Sixty-six of 75 patients (88%) had with hepatic manifestations, 39 of them had only hepatic manifestations, 27 patients had hepatic and neurological manifestations or other symptoms at the same time (16 patients had associated neurological manifestation, 3 patients had osteopathy, 8 patients had other symptoms). Eight of the 75 patients (10.7%) had only neurological symptoms, one patient (5 years old) had no symptom. Twelve changing patterns were detected in ATP7B gene by DNA sequencing, including seven mutations (R778L, C656X, G943D, V1140A, V1106I V1216M and 1384del17), six polymorphisms (IVS4-5t/c, A2495G, C2310G, IVS18 + 6c/t and IVS20 + 5a/g). R778L occurred in 49/66 patients (74%) with hepatic manifestations, homozygosis of R778L in 16 patients, heterozygosity of R778L in 33 patients. V1106I mutation of ATP7B gene occurred in 2 patients with delaying onset of clinical symptoms. Cu-ATPase activity of three patients with known mutations (R778L/ V1106I/A2495G, R778L/V1216M and R778L/R778L) were determined, and the activity of Cu-ATPase was decreased by 44.55%, 88.23% and 69.49% respectively.

CONCLUSION: 1384del17bp is a novel mutation found in WD patients. R778L is the most common mutation of ATP7B gene. There is a correlation between R778L and hepatic manifestations in WD patient.

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