학술논문
Reanalysis of exome negative patients with rare disease: a pragmatic workflow for diagnostic applications.
Document Type
Article
Author
Schobers, Gaby; Schieving, Jolanda H.; Yntema, Helger G.; Pennings, Maartje; Pfundt, Rolph; Derks, Ronny; Hofste, Tom; de Wijs, Ilse; Wieskamp, Nienke; van den Heuvel, Simone; Galbany, Jordi Corominas; Gilissen, Christian; Nelen, Marcel; Brunner, Han G.; Kleefstra, Tjitske; Kamsteeg, Erik-Jan; Willemsen, Michèl A. A. P.; Vissers, Lisenka E. L. M.
Source
Subject
*RARE diseases
*GENETIC disorder diagnosis
*ACADEMIC medical centers
*PEDIATRIC neurology
*WORKFLOW software
*GENETIC disorders
*WORKFLOW
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Language
ISSN
1756-994X
Abstract
Background: Approximately two third of patients with a rare genetic disease remain undiagnosed after exome sequencing (ES). As part of our post-test counseling procedures, patients without a conclusive diagnosis are advised to recontact their referring clinician to discuss new diagnostic opportunities in due time. We performed a systematic study of genetically undiagnosed patients 5 years after their initial negative ES report to determine the efficiency of diverse reanalysis strategies. Methods: We revisited a cohort of 150 pediatric neurology patients originally enrolled at Radboud University Medical Center, of whom 103 initially remained genetically undiagnosed. We monitored uptake of physician-initiated routine clinical and/or genetic re-evaluation (ad hoc re-evaluation) and performed systematic reanalysis, including ES-based resequencing, of all genetically undiagnosed patients (systematic re-evaluation). Results: Ad hoc re-evaluation was initiated for 45 of 103 patients and yielded 18 diagnoses (including 1 non-genetic). Subsequent systematic re-evaluation identified another 14 diagnoses, increasing the diagnostic yield in our cohort from 31% (47/150) to 53% (79/150). New genetic diagnoses were established by reclassification of previously identified variants (10%, 3/31), reanalysis with enhanced bioinformatic pipelines (19%, 6/31), improved coverage after resequencing (29%, 9/31), and new disease-gene associations (42%, 13/31). Crucially, our systematic study also showed that 11 of the 14 further conclusive genetic diagnoses were made in patients without a genetic diagnosis that did not recontact their referring clinician. Conclusions: We find that upon re-evaluation of undiagnosed patients, both reanalysis of existing ES data as well as resequencing strategies are needed to identify additional genetic diagnoses. Importantly, not all patients are routinely re-evaluated in clinical care, prolonging their diagnostic trajectory, unless systematic reanalysis is facilitated. We have translated our observations into considerations for systematic and ad hoc reanalysis in routine genetic care. [ABSTRACT FROM AUTHOR]