Normal ATXN3 Allele but Not CHIP Polymorphisms Modulates Age at Onset in Machado-Joseph Disease

Normal ATXN3 Allele but Not CHIP Polymorphisms Modulates Age at Onset in Machado-Joseph Disease

Age at onset (AO) in Machado-Joseph disease (MJD) is closely associated with the length of the CAG repeat at the mutant ATXN3 allele, but there are other intervening factors. Experimental evidence indicates that the normal ATXN3 allele and the C-terminal heat shock protein 70 (Hsp70)-interacting pro...

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Published in:Frontiers in neurology Vol. 3; p. 164
Main Authors: França, Jr, Marcondes C, Emmel, Vanessa E, D'Abreu, Anelyssa, Maurer-Morelli, Cláudia V, Secolin, Rodrigo, Bonadia, Luciana Cardoso, da Silva, Marilza Santos, Nucci, Anamarli, Jardim, Laura Bannach, Saraiva-Pereira, Maria Luiza, Marques, Jr, Wilson, Paulson, Henry, Lopes-Cendes, Iscia
Format: Journal Article
Language:English
Published: Switzerland Frontiers Media S.A 2012
Subjects:
age at onset
Machado-Joseph Disease
modifier genes
Neuroscience
PolyQ
SCA3
polyQ
SCA3
age at onset
modifier genes
Machado–Joseph disease
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Summary:Age at onset (AO) in Machado-Joseph disease (MJD) is closely associated with the length of the CAG repeat at the mutant ATXN3 allele, but there are other intervening factors. Experimental evidence indicates that the normal ATXN3 allele and the C-terminal heat shock protein 70 (Hsp70)-interacting protein (CHIP) may be genetic modifiers of AO in MJD. To investigate this hypothesis, we determined the length of normal and expanded CAG repeats at the ATXN3 gene in 210 unrelated patients with MJD. In addition, we genotyped five single nucleotide polymorphisms (SNPs) within the CHIP gene. We first compared the frequencies of the different genotypes in two subgroups of patients who were highly discordant for AO after correction for the length of the expanded CAG allele. The possible modifier effect of each gene was then evaluated in a stepwise multiple linear regression model. AO was associated with the length of the expanded CAG allele (r(2) = 0.596, p < 0.001). Frequencies of the normal CAG repeats at the ATXN3 gene and of CHIP polymorphisms did not differ significantly between groups with highly discordant ages at onset. However, addition of the normal allele improved the model fit for prediction of AO (r(2) = 0.604, p = 0.014). Indeed, we found that the normal CAG allele at ATXN3 had a positive independent effect on AO. The normal CAG repeat at the ATXN3 gene has a small but significant influence on AO of MJD.
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This article was submitted to Frontiers in Neurogenomics, a specialty of Frontiers in Neurology.
Edited by: Hua Lou, Case Western Reserve University, USA
Reviewed by: Mengqing Xiang, UMDNJ-Robert Wood Johnson Medical School, USA; Eng-King Tan, National Neuroscience Institute, Singapore
ISSN:1664-2295
1664-2295
DOI:10.3389/fneur.2012.00164