Screening and cell-based assessment of mutations in the Aristaless-related homeobox (ARX) gene

T. Fullston; M. Finnis; A. Hackett; B. Hodgson; L. Brueton; G. Baynam; A. Norman; O. Reish; C. Shoubridge; J. Gecz

doi:10.1111/j.1399-0004.2011.01685.x

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Screening and cell-based assessment of mutations in the Aristaless-related homeobox (ARX) gene

Journal article

Peer reviewed

Screening and cell-based assessment of mutations in the Aristaless-related homeobox (ARX) gene

T. Fullston, M. Finnis, A. Hackett, B. Hodgson, L. Brueton, G. Baynam, A. Norman, O. Reish, C. Shoubridge and J. Gecz

Clinical Genetics, Vol.80(6), pp.510-522

2011

DOI: https://doi.org/10.1111/j.1399-0004.2011.01685.x

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Abstract

ARX mutations cause a diverse spectrum of human disorders, ranging from severe brain and genital malformations to non-syndromic intellectual disability (ID). ARX is a transcription factor with multiple domains that include four polyalanine (pA) tracts, the first two of which are frequently expanded by mutations. We progressively screened DNA samples from 613 individuals with ID initially for the most frequent ARX mutations (c.304ins(GCG)7‘expansion’ of pA1 and c.429_452dup ‘dup24bp’ of pA2). Five hundred samples without pA1 or pA2 mutations had the entire ARX ORF screened by single stranded polymorphism conformation (SSCP) and/or denaturing high pressure liquid chromatography (dHPLC) analysis. Overall, eight families with six mutations in ARX were identified (1.31%): five duplication mutations in pA2 (0.82%) with three new clinical reports of families with the dup24bp and two duplications larger than the dup24bp mutation discovered (dup27bp, dup33bp); and three point mutations (0.6%), including one novel mutation in the homeodomain (c.1074G>T). Four ultraconserved regions distal to ARX (uc466–469) were also screened in a subset of 94 patients, with three unique nucleotide changes identified in two (uc466, uc467). The subcellular localization of full length ARX proteins was assessed for 11 variants. Protein mislocalization increased as a function of pA2 tract length and phenotypic severity, as has been previously suggested for pA1. Similarly, protein mislocalization of the homeodomain mutations also correlated with clinical severity, suggesting an emerging genotype vs cellular phenotype correlation.

Details

Title: Screening and cell-based assessment of mutations in the Aristaless-related homeobox (ARX) gene
Authors/Creators: T. Fullston (Author/Creator) - Women's and Children's Hospital
M. Finnis (Author/Creator) - Women's and Children's Hospital
A. Hackett (Author/Creator) - Hunter Genetics
B. Hodgson (Author/Creator) - Women's and Children's Hospital
L. Brueton (Author/Creator) - Birmingham Women's Hospital
G. Baynam (Author/Creator) - The University of Western Australia
A. Norman (Author/Creator) - Birmingham Women's Hospital
O. Reish (Author/Creator) - Assaf Harofeh Medical Center
C. Shoubridge (Author/Creator) - Women's and Children's Hospital
J. Gecz (Author/Creator) - The University of Adelaide
Publication Details: Clinical Genetics, Vol.80(6), pp.510-522
Publisher: Wiley-Blackwell
Identifiers: 991005542465707891
Murdoch Affiliation: Murdoch University
Language: English
Resource Type: Journal article

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Collaboration types: Domestic collaboration; International collaboration
Citation topics: 1 Clinical & Life Sciences; 1.186 Chromosome Disorders; 1.186.1479 Fragile X Syndrome
Web Of Science research areas: Genetics & Heredity
ESI research areas: Clinical Medicine