J Pediatr Genet 2023; 12(03): 206-212
DOI: 10.1055/s-0041-1736610
Original Article

The Efficacy of Whole Genome Sequencing and RNA-Seq in the Diagnosis of Whole Exome Sequencing Negative Patients with Complex Neurological Phenotypes

1   Department of Pediatrics, John R. Oishei Children's Hospital, New York, United States
,
Lauren I. Brady
2   Department of Pediatrics, McMaster University Medical Centre, Ontario, Canada
,
3   Praxis Genomics, Atlanta, Georgia, United States
,
3   Praxis Genomics, Atlanta, Georgia, United States
,
2   Department of Pediatrics, McMaster University Medical Centre, Ontario, Canada
› Author Affiliations
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Abstract

Whole-genome sequencing (WGS) is being increasingly utilized for the diagnosis of neurological disease by sequencing both the exome and the remaining 98 to 99% of the genetic code. In addition to more complete coverage, WGS can detect structural variants (SVs) and intronic variants (SNVs) that cannot be identified by whole exome sequencing (WES) or chromosome microarray (CMA). Other multi-omics tools, such as RNA sequencing (RNA-Seq), can be used in conjunction with WGS to functionally validate certain variants by detecting changes in gene expression and splicing. The objective of this retrospective study was to measure the diagnostic yield of duo/trio-based WGS and RNA-Seq in a cohort of 22 patients (20 families) with pediatric onset neurological phenotypes and negative or inconclusive WES results in lieu of reanalysis. WGS with RNA-Seq resulted in a definite diagnosis of an additional 25% of cases. Sixty percent of these solved cases arose from the identification of variants that were missed by WES. Variants that could not be unequivocally proven to be causative of the patients' condition were identified in an additional 5% of cases.

Supplementary Material



Publication History

Received: 16 March 2021

Accepted: 20 September 2021

Article published online:
09 November 2021

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