Cox Dw scite author profile

In the present study we examined 33 German and 10 Cuban unrelated Wilson disease (WND) index patients and their relatives. The common His1069Gln mutation accounted for 42% of all WND chromosomes in the German series and the haplotype C was found to be highly predictive for this mutation. Six WND gene mutations have not been described previously and involved a splice site at intron 18 (3903 + del1G), a termination codon in the copper-binding region of exon 2 (Cys271X), and missense mutations in transmembrane region 2 (Gly710Ala), in transmembrane region 3 (Tyr741Cys), in the DKTGT motif (Thr1031Ile) and in the ATP loop region (Gly1176Arg). In 15 German WND index patients and three sibs both WND mutations could be determined and a genotype-phenotype correlation was attempted. Patients homozygous for the His1069Gln mutation showed almost the complete range of clinical presentations, and thus in our study this mutation is not associated with a late, neurological presentation.

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Genetic variation in the promoter and 5′ UTR of the copper transporter, ATP7B, in patients with Wilson disease

Cullen

Prat

2003

Clinical Genetics

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ATP7B is a copper-transporting P-type ATPase defective in the copper transport disorder, Wilson disease (WND). We have sequenced the 5' UTR and promoter region of ATP7B in 37 unrelated WND patients in whom partial sequencing of the coding region and intron/exon boundaries of the gene had failed to identify one or both disease-causing mutations. Three patients were found to be heterozygous for a 15 bp deletion between nucleotides -424 and -441. This deletion had been previously identified as the most common mutation in Sardinian WND patients. Two novel single-nucleotide changes were also identified within the 5' UTR and promoter of ATP7B; however, these were found at a similar frequency in control chromosomes and are apparently normal variants. These results suggest that mutations in regulatory elements of ATP7B are uncommon in patients of European ancestry, except in Sardinia.

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COMMD1 (MURR1) as a candidate in patients with copper storage disease of undefined etiology

Coronado¹,

Bonneville²,

Nazer³

et al. 2005

Clinical Genetics

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Cox Dw

Report of nomenclature meeting for α1-antitrypsin

His1069Gln and six novel Wilson disease mutations: analysis of relevance for early diagnosis and phenotype

Genetic variation in the promoter and 5′ UTR of the copper transporter, ATP7B, in patients with Wilson disease

COMMD1 (MURR1) as a candidate in patients with copper storage disease of undefined etiology

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