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Molecular Investigations to Improve Diagnostic Accuracy in Patients With ARC Syndrome
Cited 24 time in
Web of Science
Cited 27 time in Scopus
- Authors
- Issue Date
- 2009-02
- Publisher
- WILEY-LISS
- Citation
- HUMAN MUTATION; Vol.30 2; E330-E337
- Keywords
- arthrogryposis ; neonatal cholestasis ; vesicular trafficking defect ; ARC ; renal tubular dysfunction
- Abstract
- Arthrogryposis, Renal dysfunction and Cholestasis (ARC) syndrome is a multi-system autosomal recessive disorder caused by germline mutations in VPS33B. The detection of germline VPS33B mutations removes the need for diagnostic organ biopsies (these carry a >50% risk of life-threatening haemorrhage due to platelet dysfunction); however, VPS33B mutations are not detectable in similar to 25% of patients. In order further to define the molecular basis of ARC we performed mutation analysis and mRNA and protein studies in patients with a clinical diagnosis of ARC. Here we report novel mutations in VPS33B in patients from Eastern Europe and South East Asia. One of the mutations was present in 7 unrelated Korean patients. Reduced expression of VPS33B and cellular phenotype was detected in fibroblasts from patients clinically diagnosed with ARC with and without known VPS33B mutations. One mutation-negative patient was found to have normal mRNA and protein levels. This patient`s clinical condition improved and he is alive at the age of 2.5 years. Thus we show that all patients with a classical clinical course of ARC had decreased expression of VPS33B whereas normal VPS33B expression was associated with good prognosis despite initial diagnosis of ARC. (C) 2008 Wiley-Liss, Inc.
- ISSN
- 1059-7794
- Language
- English
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