Partially methylated alleles, microdeletion, and tissue mosaicism in a fragile X male with tremor and ataxia at 30 years of age: a case report

Hwang, Yun Tae; Aliaga, Solange Mabel; Heard, Robert; Godler, David Eugeny; Arpone, Marta; Francis, David; Li, Xin; Chong, Belinda; Slater, Howard Robert; Rogers, Carolyn; Bretherton, Lesley; Hunter, Matthew

Title: Partially methylated alleles, microdeletion, and tissue mosaicism in a fragile X male with tremor and ataxia at 30 years of age: a case report
Creator: Hwang, Yun Tae; Aliaga, Solange Mabel; Heard, Robert; Godler, David Eugeny; Arpone, Marta; Francis, David; Li, Xin; Chong, Belinda; Slater, Howard Robert; Rogers, Carolyn; Bretherton, Lesley; Hunter, Matthew
Relation: NHMRC.1017263, NHMRC.1104299 http://purl.org/au-research/grants/nhmrc/1103389 & NHMRC.1103389
Relation: American Journal of Medical Genetics: Part A Vol. 170, Issue 12, p. 3327-3332
Publisher Link: http://dx.doi.org/10.1002/ajmg.a.37954
Publisher: John Wiley & Sons
Resource Type: journal article
Date: 2016
Description: CGG repeat expansion >200 within FMR1, termed full mutation (FM), has been associated with promoter methylation, consequent silencing of gene expression and fragile X syndrome (FXS)-a common cause of intellectual disability and co-morbid autism. Unmethylated premutation (55-199 repeats) and FM alleles have been associated with fragile X related tremor/ataxia syndrome (FXTAS), a late onset neurodegenerative disorder. Here we present a 33-year-old male with FXS, with white matter changes and progressive deterioration in gait with cerebellar signs consistent with probable FXTAS; there was no evidence of any other cerebellar pathology. We show that he has tissue mosaicism in blood, saliva, and buccal samples for the size and methylation of his expanded alleles and a de novo, unmethylated microdeletion. This microdeletion involves a ~80 bp sequence in the FMR1 promoter as well as complete loss of the CGG repeat in a proportion of cells. Despite FMR1 mRNA levels in blood within the normal range, the methylation and CGG sizing results are consistent with the diagnosis of concurrent FXS and probable FXTAS. The demonstrated presence of unmethylated FM alleles would explain the manifestation of milder than expected cognitive and behavioral impairments and early onset of cerebellar ataxia. Our case suggests that individuals with FXS, who manifest symptoms of FXTAS, may benefit from more detailed laboratory testing.
Subject: Fragile X syndrome; fragile X related tremor/ataxia syndrome; tremor; cerebellar ataxia; mental retardation; molecular biology; methylation; mosaicism
Identifier: http://hdl.handle.net/1959.13/1339287
Identifier: uon:28217
Identifier: ISSN:1552-4825
Language: eng
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