Consistency of variant interpretations among bioinformaticians and clinical geneticists in hereditary cancer panels

Consistency of variant interpretations among bioinformaticians and clinical geneticists in hereditary cancer panels

Next-generation sequencing (NGS) is used increasingly in hereditary cancer patients' (HCP) management. While enabling evaluation of multiple genes simultaneously, the technology brings to light the dilemma of variant interpretation. Here, we aimed to reveal the underlying reasons for the discre...

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Bibliographic Details
Published in:European journal of human genetics : EJHG Vol. 30; no. 3; pp. 378 - 383
Main Authors: Agaoglu, Nihat Bugra, Unal, Busra, Akgun Dogan, Ozlem, Kanev, Martin Orlinov, Zolfagharian, Payam, Ozemri Sag, Sebnem, Temel, Sehime Gulsun, Doganay, Levent
Format: Journal Article
Language:English
Published: England Nature Publishing Group 01-03-2022
Springer International Publishing
Subjects:
BRCA1 protein
Cancer
Discordance
Genetic Predisposition to Disease
High-Throughput Nucleotide Sequencing
Humans
Mutation
Neoplasms - genetics
Next-generation sequencing
Patients
Precision medicine
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Summary:Next-generation sequencing (NGS) is used increasingly in hereditary cancer patients' (HCP) management. While enabling evaluation of multiple genes simultaneously, the technology brings to light the dilemma of variant interpretation. Here, we aimed to reveal the underlying reasons for the discrepancy in the evidence titles used during variant classification according to ACMG guidelines by two different bioinformatic specialists (BIs) and two different clinical geneticists (CGs). We evaluated final reports of 1920 cancer patients and 189 different variants from 285 HCP were enrolled to the study. A total of 173 of these variants were classified as pathogenic (n = 132) and likely pathogenic (n = 41) by the BI and an additional 16 variants, that were classified as VUS by at least one interpreter and their classification would change the clinical management, were compared for their evidence titles between different specialists. The attributed evidence titles and the final classification of the variants among BIs and CGs were compared. The discrepancy between P/LP final reports was 22.5%. The discordance between CGs was 30% whereas the discordance between two BIs was almost 75%. The use of PVS1, PS3, PP3, PP5, PM1, PM2, BP1, BP4 criteria markedly varied from one expert to another. This difference was particularly noticeable in PP3, PP5, and PM1 evidence and mostly in the variants affecting splice sites like BRCA1(NM_007294.4) c.4096 + 1 G > A and CHEK2(NM_007194.4) c.592 + 3 A > T. With recent advancements in precision medicine, the importance of variant interpretations is emerging. Our study shows that variant interpretation is subjective process that is in need of concrete definitions for accurate and standard interpretation.
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ISSN:1018-4813
1476-5438
1476-5438
DOI:10.1038/s41431-022-01060-7