Comprehensive prenatal diagnostics: Exome versus genome sequencing.

Abstract

This study aimed to assess the diagnostic yield of prenatal genetic testing using trio whole exome sequencing (WES) and trio whole genome sequencing (WGS) in pregnancies with fetal anomalies, comparing the results to conventional chromosomal microarray (CMA) analysis. A total of 40 pregnancies with fetal anomalies or increased nuchal translucency (NT≥5mm) were included between the 12th and 21st week of gestation. Trio WES/WGS and CMA were performed on all cases. The trio WES/WGS analysis increased the diagnostic yield by 25% in cases with negative CMA results. Furthermore, all six chromosomal aberrations identified by CMA were independently detected by WES/WGS analysis. In total, 16 out of 40 cases obtained a genetic sequence variant, copy number variant or aneuploidy explaining the phenotype, resulting in an overall WES/WGS diagnostic yield of 40%. WES analysis provided a more reliable identification of mosaic sequence variants than WGS due to higher sequencing depth. Prenatal WES/WGS proved to be powerful diagnostic tools for fetal anomalies, surpassing the diagnostic yield of CMA. They have the potential to serve as standalone methods for prenatal diagnosis. The study highlighted the limitations of WGS in accurately detecting mosaic variants, which is particularly relevant when analyzing chorionic villus samples. This article is protected by copyright. All rights reserved.