Clinical validity assessment of genes for inclusion in multi-gene panel testing: A systematic approach.

Tricia N Zion,Bess Wayburn,Sourat Darabi,Devon Lamb Thrush,Erica D Smith,Tami Johnston, Brissa Martin,Kelly D F Hagman, Melissa Parra, Christian Antolik

MOLECULAR GENETICS & GENOMIC MEDICINE(2019)

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Abstract
BackgroundAdvances in sequencing technology have led to expanded use of multi-gene panel tests (MGPTs) for clinical diagnostics. Well-designed MGPTs must balance increased detection of clinically significant findings while mitigating the increase in variants of uncertainsignificance (VUS). To maximize clinical utililty, design of such panels should include comprehensive gene vetting using a standardized clinical validity (CV) scoring system. MethodsTo assess the impact of CV-based gene vetting on MGPT results, data from MGPTs for cardiovascular indications were retrospectively analyzed. Using our CV scoring system, genes were categorized as having definitive, strong, moderate, or limited evidence. The rates of reported pathogenic or likely pathogenic variants and VUS were then determined for each CV category. ResultsOf 106 total genes, 42% had definitive, 17% had strong, 29% had moderate, and 12% had limited CV. The detection rate of variants classified as pathogenic or likely pathogenic was higher for genes with greater CV, while the VUS rate showed an inverse relationship with CV score. No pathogenic or likely pathogenic findings were observed in genes with a limited CV. ConclusionThese results demonstrate the importance of a standardized, evidence-based vetting process to establish CV for genes on MGPTs. Using our proposed system may help to increase the detection rate while mitigating higher VUS rates.
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Key words
cardiology,clinical validity,detection rate,gene characterization,gene vetting,gene-disease relationship,multi-gene panel genetic testing
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