A semiautomated whole-exome sequencing workflow leads to increased diagnostic yield and identification of novel candidate variants

Author:

Ji Jianling,Shen Lishuang,Bootwalla Moiz,Quindipan Catherine,Tatarinova Tatiana,Maglinte Dennis T.,Buckley Jonathan,Raca Gordana,Saitta Sulagna C.,Biegel Jaclyn A.,Gai Xiaowu

Abstract

Advancing the clinical utility of whole-exome sequencing (WES) for patients with suspected genetic disorders is largely driven by bioinformatics approaches that streamline data processing and analysis. Herein, we describe our experience with implementing a semiautomated and phenotype-driven WES diagnostic workflow, incorporating both the DRAGEN pipeline and the Exomiser variant prioritization tool, at an academic children's hospital with an ethnically diverse pediatric patient population. We achieved a 41% molecular diagnostic rate for 66 duo-, quad-, or trio-WES cases, and 28% for 40 singleton-WES cases. Preliminary results were returned to ordering physicians within 1 wk for 12 of 38 (32%) probands with positive findings, which were instrumental in guiding the appropriate clinical management for a variety of patients, especially in critical care settings. The semiautomated and streamlined WES workflow also enabled us to identify novel variants in candidate disease genes in patients with developmental delay and autism and immune disorders and cancer, including ANK2, BPTF, BCL11A, FOXN1, PLAA, ATRX, DNAJC21, and RAD50. Together, we demonstrated the implementation of a streamlined WES workflow that was successfully applied for both clinical and research purposes.

Publisher

Cold Spring Harbor Laboratory

Subject

General Medicine

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