Clinical validity assessment of genes frequently tested on hereditary breast and ovarian cancer susceptibility sequencing panels
Menée à l'aide des méthodes d'analyse du groupe de travail du "Clinical Genome Resource", cette étude évalue le niveau d'association entre des gènes de prédisposition au cancer, fréquemment ciblés par les tests génétiques, et le risque de cancer héréditaire du sein ou de l'ovaire
Purpose : Several genes on hereditary breast and ovarian cancer susceptibility test panels have not been systematically examined for strength of association with disease. We employed the Clinical Genome Resource (ClinGen) clinical validity framework to assess the strength of evidence between selected genes and breast or ovarian cancer.
Methods : Thirty-one genes offered on cancer panel testing were selected for evaluation. The strength of gene–disease relationship was systematically evaluated and a clinical validity classification of either Definitive, Strong, Moderate, Limited, Refuted, Disputed, or No Reported Evidence was assigned.
Results : Definitive clinical validity classifications were made for 10/31 and 10/32 gene–disease pairs for breast and ovarian cancer respectively. Two genes had a Moderate classification whereas, 6/31 and 6/32 genes had Limited classifications for breast and ovarian cancer respectively. Contradictory evidence resulted in Disputed or Refuted assertions for 9/31 genes for breast and 4/32 genes for ovarian cancer. No Reported Evidence of disease association was asserted for 5/31 genes for breast and 11/32 for ovarian cancer.
Conclusion : Evaluation of gene–disease association using the ClinGen clinical validity framework revealed a wide range of classifications. This information should aid laboratories in tailoring appropriate gene panels and assist health-care providers in interpreting results from panel testing.
Genetics in Medicine , résumé, 2018