The clinical value of optical genome mapping in the rapid characterization of RB1 duplication and 15q23q24.2 triplication, for more appropriate prenatal genetic counselling

Author:

Bouassida Malek1ORCID,Molina‐Gomes Denise1,Koraichi Fairouz1,Hervé Bérénice1,Lhuilier Morgane1,Duvillier Clémence2,Le Gall Jessica3,Gauthier‐Villars Marion3,Serazin Valérie1ORCID,Quibel Thibaud2,Dard Rodolphe14,Vialard François14

Affiliation:

1. Genetics Department CHI de Poissy‐St Germain en Laye Poissy France

2. Obstetrics Department CHI de Poissy‐St Germain en Laye Poissy France

3. Genetics Department Institut Curie Paris France

4. RHuMA Team UMR‐BREED, UVSQ, INRAE, ENVA Montigny le Bretonneux France

Abstract

AbstractBackgroundDespite recent advances in prenatal genetic diagnosis, medical geneticists still face considerable difficulty in interpreting the clinical outcome of copy‐number‐variant duplications and defining the mechanisms underlying the formation of certain chromosomal rearrangements.Optical genome mapping (OGM) is an emerging cytogenomic tool with proved ability to identify the full spectrum of cytogenetic aberrations.MethodsHere, we report on the use of OGM in a prenatal diagnosis setting. Detailed breakpoint mapping was used to determine the relative orientations of triplicated and duplicated segments in two unrelated foetuses harbouring chromosomal aberrations: a de novo 15q23q24.2 triplication and a paternally inherited 13q14.2 duplication that overlapped partially with the RB1 gene.ResultsOGM enabled us to suggest a plausible mechanism for the triplication and confirmed that the RB1 duplication was direct oriented and in tandem. This enabled us to predict the pathogenic consequences, refine the prognosis and adapt the follow‐up and familial screening appropriately.ConclusionAlong with an increase in diagnostic rates, OGM can rapidly highlight genotype–phenotype correlations, improve genetic counselling and significantly influence prenatal management.

Publisher

Wiley

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