Fragile X Syndrome Caused by Maternal Somatic Mosaicism of FMR1 Gene: Case Report and Literature Review

Author:

Gómez-Rodríguez Maria Jose,Morales-Conejo Montserrat,Arteche-López Ana,Sánchez-Calvín Maria TeresaORCID,Quesada-Espinosa Juan FranciscoORCID,Gómez-Manjón IreneORCID,Palma-Milla CarmenORCID,Lezana-Rosales Jose MiguelORCID,Pérez de la Fuente RubenORCID,Martin-Ramos Maria-Luisa,Fernández-Guijarro Manuela,Moreno-García Marta,Alvarez-Mora Maria IsabelORCID

Abstract

Fragile X syndrome (FXS) is caused by an abnormal expansion of the number of trinucleotide CGG repeats located in the 5′ UTR in the first exon of the FMR1 gene. Size and methylation mosaicisms are commonly observed in FXS patients. Both types of mosaicisms might be associated with less severe phenotypes depending on the number of cells expressing FMRP. Although this dynamic mutation is the main underlying cause of FXS, other mechanisms, including point mutations or deletions, can lead to FXS. Several reports have demonstrated that de novo deletions including the entire or a portion of the FMR1 gene end up with the absence of FMRP and, thus, can lead to the typical clinical features of FXS. However, very little is known about the clinical manifestations associated with FMR1 gene deletions in mosaicism. Here, we report an FXS case caused by an entire hemizygous deletion of the FMR1 gene caused by maternal mosaicism. This manuscript reports this case and a literature review of the clinical manifestations presented by carriers of FMR1 gene deletions in mosaicism.

Funder

Fundación Mutua Madrileña

Fundación Merck Salud

Agency for Administration of University and Research

Publisher

MDPI AG

Subject

Genetics (clinical),Genetics

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