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Comparison of first‐tier whole‐exome sequencing with a multi‐step traditional approach for diagnosing paediatric outpatients: An Italian prospective study.

Authors :
Rosina, Erica
Pezzani, Lidia
Apuril, Erika
Pezzoli, Laura
Marchetti, Daniela
Bellini, Matteo
Lucca, Camilla
Meossi, Camilla
Massimello, Marta
Mariani, Milena
Scatigno, Agnese
Cattaneo, Elisa
Colombo, Lorenzo
Maitz, Silvia
Cereda, Anna
Milani, Donatella
Spaccini, Luigina
Bedeschi, Maria Francesca
Selicorni, Angelo
Iascone, Maria
Source :
Molecular Genetics & Genomic Medicine. Jan2024, Vol. 12 Issue 1, p1-12. 12p.
Publication Year :
2024

Abstract

Background: The recent guidelines suggest the use of genome‐wide analyses, such as whole exome sequencing (WES), at the beginning of the diagnostic approach for cases with suspected genetic conditions. However, in many realities it still provides for the execution of a multi‐step pathway, thus requiring several genetic tests to end the so‐called 'diagnostic odyssey'. Methods: We reported the results of GENE Project (Genomic analysis Evaluation NEtwork): a multicentre prospective cohort study on 125 paediatric outpatients with a suspected genetic disease in which we performed first‐tier trio‐WES, including exome‐based copy number variation analysis, in parallel to a 'traditional approach' of two/three sequential genetic tests. Results: First‐tier trio‐WES detected a conclusive diagnosis in 41.6% of patients, way above what was found with routine genetic testing (25%), with a time‐to‐result of about 50 days. Notably, the study showed that 44% of WES‐reached diagnoses would be missed with the traditional approach. The diagnostic rate (DR) of the two approaches varied in relation to the phenotypic class of referral and to the proportion of cases with a defined diagnostic suspect, proving the major difference for neurodevelopmental disorders. Moreover, trio‐WES analysis detected variants in candidate genes of unknown significance (EPHA4, DTNA, SYNCRIP, NCOR1, TFDP1, SPRED3, EDA2R, PHF12, PPP1R12A, WDR91, CDC42BPG, CSNK1D, EIF3H, TMEM63B, RIPPLY3) in 19.4% of undiagnosed cases. Conclusion: Our findings represent real‐practice evidence of how first‐tier genome‐wide sequencing tests significantly improve the DR for paediatric outpatients with a suspected underlying genetic aetiology, thereby allowing a time‐saving setting of the correct management, follow‐up and family planning. [ABSTRACT FROM AUTHOR]

Details

Language :
English
ISSN :
23249269
Volume :
12
Issue :
1
Database :
Academic Search Index
Journal :
Molecular Genetics & Genomic Medicine
Publication Type :
Academic Journal
Accession number :
175072123
Full Text :
https://doi.org/10.1002/mgg3.2316