Tandem Triplication 11p15.5-ICR1 (<i>H19/IGF2</i>) Detected by Microarray and Optical Genome Mapping in a Prenatal Beckwith-Wiedemann Case

Author:

Lloveras Elisabet,Pérez Cristina,Mendez Begoña,Martin Susana,Alves Claudia,Reis-Lima Margarida

Abstract

Optical genome mapping (OGM) appears as a new tool for matching standard cytogenetic methods (karyotype and microarray) into a single assay. The chromosomal region 11p15.5 harbours two differentially methylated regions, the imprinting centre regions 1 and 2 (ICR1, ICR2). Disturbances in both regions alter human growth and are associated with two imprinting disorders, Beckwith-Wiedemann (BWS) and Silver-Russell syndromes. Herein, we present a prenatal case with a triplication in 11p15.5, including the <i>H19/IGF2</i> imprinted region, detected by microarray and OGM. A 30‐year‐old pregnant woman of 17 weeks of gestation was referred for prenatal karyotype and microarray study because of increased nuchal translucency, short femur, megabladder, hyperechogenic bowel, and renal ectasia. Microarray, OGM, and MS-MLPA were performed, and a tandem <i>cis</i>-triplication in 11p15.5 and hypermethylation of the ICR1 region, compatible with BWS was detected. OGM, with its power to detect all classes of structural variants, including copy number variants, at a higher resolution than traditional cytogenetic methods can play a significant role in prenatal care and management as a next-generation cytogenomic tool. This study further supports the hypotheses that the amplification/duplication-triplication of the <i>H19/IGF2</i> region could be related to BWS if it is of paternal origin.

Publisher

S. Karger AG

Subject

Genetics (clinical),Genetics,Molecular Biology

Reference6 articles.

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