| Article ID | Journal | Published Year | Pages | File Type |
|---|---|---|---|---|
| 5906330 | Gene | 2013 | 5 Pages |
â¢Report of a female foetus mosaic for full mutation/intermediate allele of FMR1 geneâ¢Postzygotic expansion mechanism of a maternal premutation into a full mutationâ¢Subsequent full mutation regression to intermediate allele in a proportion of cellsâ¢Postzygotic retraction event in early embryogenesisâ¢Retraction before the commitment of cells into the different tissues
Fragile X syndrome is caused by the expansion of an unstable CGG repeat in the 5â²UTR of FMR1 gene. The occurrence of mosaicism is not uncommon, especially in male patients, whereas in females it is not so often reported. Here we report a female foetus that was subject to prenatal diagnosis, because of her mother being a premutation carrier. The foetus was identified as being a mosaic for an intermediate allele and a full mutation of FMR1 gene, in the presence of a normal allele. The mosaic status was confirmed in three different tissues of the foetus - amniotic fluid, skin biopsy and blood - the last two obtained after pregnancy termination. Karyotype analysis and X-chromosome STR markers analysis do not support the mosaicism as inheritance of both maternal alleles. Oligonucleotide array-CGH excluded an imbalance that could contain the primer binding site with a different repeat size. The obtained results give compelling evidence for a postzygotic expansion mechanism where the foetus mosaic pattern originated from expansion of the mother's premutation into a full mutation and consequent regression to an intermediate allele in a proportion of cells. These events occurred in early embryogenesis before the commitment of cells into the different tissues, as the three tested tissues of the foetus have the same mosaic pattern. The couple has a son with Fragile X mental retardation syndrome and choose to terminate this pregnancy after genetic counselling.
