Reduction in nuclear speckles and transcriptome de-regulation in fibroblast of intellectually disabled patients with mutations at the FRAXE site

GSE27953

Homo sapiens

12 Downloadable Samples

Affymetrix Human Human Exon 1.0 ST Array (huex10st)

Submitter Supplied Information

Description

Loss of function of FMR2 due to either hypermethylation of the CpG island as a consequence of the expansion of the CCG repeat near its transcription start site, or internal deletion of FMR2 is considered to be the major cause of FRAXE fragile site associated intellectual disability. FMR2 was shown to be a potent transcription activator as well as an RNA binding protein capable of regulating alternative splicing.

PubMed ID

23562910

Publication Title

Loss of FMR2 further emphasizes the link between deregulation of immediate early response genes FOS and JUN and intellectual disability.

Total Samples

Submitter’s Institution

SA Pathology

Authors

Melko M, Nguyen LS, Shaw M, Jolly L, Bardoni B, Gecz J

Source Repository

Gene Expression Omnibus (GEO)

Alternate Accession IDs

E-GEOD-27953

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