Skip to main content
OSTI.GOVU.S. Department of Energy Office of Scientific and Technical Information
U.S. Department of Energy
Office of Scientific and Technical Information
 

The Wilson disease gene: Haplotypes and mutations

Journal Article · · American Journal of Human Genetics
OSTI ID:134342
; ;  [1];  [2]
  1. Hospital for Sick Children, Toronto (Canada)
  2. Middlesex Hospital, London (United Kingdom)
+ Show Author Affiliations
Wilson disease (WND) is an autosomal recessive defect of copper transport. The gene involved in WND, located on chromosome 13, has recently been shown to be a putative copper transporting P-type ATPase, designated ATP7B. The gene is highly similar to ATP7A, located on the X chromosome, which is defective in Menkes disease, another disorder of copper transport. We have available for study WND families from Canada (34 families), the United Kingdom (32 families), Japan (4 families), Iceland (3 families) and Hong Kong (2 families). We have utilized four highly polymorphic CA repeat markers (D13S296, D13S301, D13S314 and D13S316) surrounding the ATP7B locus to construct haplotypes in these families. Analysis indicates that there are many unique WND haplotypes not present on normal chromosomes and that there may be a large number of different WND mutations. We have screened the WND patients for mutations in the ATP7B gene. Fifty six patients, representing all of the identified haplotypes, have been screened using single strand conformational polymorphism (SSCP), followed by selective sequencing. To date, 19 mutations and 12 polymorphisms have been identified. All of the changes are nucleotide substitutions or small insertions/deletions and there is no evidence for larger deletions as seen in the similar gene on the X chromosome, ATP7A. Haplotypes of close markers and the ability to detect some of the mutations present in the gene allow for more reliable molecular diagnosis of presymptomatic sibs of WND patients. A reassessment of individuals previously diagnosed in the presymptomatic phase is now required, as we have have identified some heterozygotes who are biochemically indistinguishable from affected homozygotes. The identification of specific mutations will soon allow direct diagnosis of WND patients with a high level of certainty.
OSTI ID:
134342
Report Number(s):
CONF-941009--
Journal Information:
American Journal of Human Genetics, Journal Name: American Journal of Human Genetics Journal Issue: Suppl.3 Vol. 55; ISSN AJHGAG; ISSN 0002-9297
Country of Publication:
United States
Language:
English

Similar Records

Haplotype studies in Wilson disease
Journal Article · Fri Dec 31 23:00:00 EST 1993 · American Journal of Human Genetics; (United States) · OSTI ID:5052743
Haplotypes and mutations in Wilson disease
Journal Article · Thu Jun 01 00:00:00 EDT 1995 · American Journal of Human Genetics · OSTI ID:91186
Analysis of mutations in Menkes and X-linked cutis laxa patients
Journal Article · Thu Sep 01 00:00:00 EDT 1994 · American Journal of Human Genetics · OSTI ID:134196

Related Subjects

55 BIOLOGY AND MEDICINE
BASIC STUDIES
ATP-ASE
BIOLOGICAL MARKERS
COPPER
DIAGNOSIS
GENE MUTATIONS
GENES
GENETIC MAPPING
HEREDITARY DISEASES
HUMAN CHROMOSOME 13
METABOLIC DISEASES
METABOLISM
NUCLEOTIDES
PATIENTS
RECESSIVE MUTATIONS
SCREENING