Authors
Peter Bauer, Krishna Kumar Kandaswamy, Maximilian ER Weiss, Omid Paknia, Martin Werber, Aida M Bertoli-Avella, Zafer Yüksel, Malgorzata Bochinska, Gabriela E Oprea, Shivendra Kishore, Volkmar Weckesser, Ellen Karges, Arndt Rolfs
Publication date
2019/1/1
Journal
Genetics in Medicine
Volume
21
Issue
1
Pages
53-61
Publisher
Elsevier
Description
Purpose
Next-generation sequencing (NGS) is rapidly replacing Sanger sequencing in genetic diagnostics. Sensitivity and specificity of NGS approaches are not well-defined, but can be estimated from applying NGS and Sanger sequencing in parallel. Utilizing this strategy, we aimed at optimizing exome sequencing (ES)–based diagnostics of a clinically diverse patient population.
Methods
Consecutive DNA samples from unrelated patients with suspected genetic disease were exome-sequenced; comparatively nonstringent criteria were applied in variant calling. One thousand forty-eight variants in genes compatible with the clinical diagnosis were followed up by Sanger sequencing. Based on a set of variant-specific features, predictors for true positives and true negatives were developed.
Results
Sanger sequencing confirmed 81.9% of ES-derived variants. Calls from the lower end of stringency accounted for the …
Scholar articles
P Bauer, KK Kandaswamy, MER Weiss, O Paknia… - Genetics in Medicine, 2019