Germline FFPE inherited cancer panel testing in deceased family members: implications for clinical management of unaffected relatives

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作者
Sarah Bennett
Elizabeth Alexander
Harry Fraser
Naomi Bowers
Andrew Wallace
Emma R. Woodward
Fiona Lalloo
Anne Marie Quinn
Shuwen Huang
Helene Schlecht
D. Gareth Evans
机构
[1] Manchester University NHS Foundation Trust,Clinical Genetics Service, Manchester Centre for Genomic Medicine, St Mary’s Hospital
[2] Auckland City Hospital,Northern Regional Genetic Service, Genetics Health Service New Zealand
[3] Manchester University NHS Foundation Trust,North West Genomic Laboratory Hub, Manchester Centre for Genomic Medicine, St Mary’s Hospital
[4] Health Innovation Manchester,Division of Evolution and Genomic Sciences, School of Biological Sciences, Faculty of Biology, Medicine and Health
[5] University of Manchester,Department of Anatomic Pathology
[6] Health innovation Manchester,undefined
[7] University Hospital Galway,undefined
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摘要
Where previously, germline genetic testing in deceased affected relatives was not possible due to the absence of lymphocytic DNA, the North-West-Genomic-Laboratory Hub (NWGLH) has developed and validated next-generation sequencing based gene panels utilising formalin-fixed-paraffin-embedded (FFPE) tissue DNA from deceased individuals. This technology has been utilised in the clinical setting for the management of unaffected relatives seen in the Clinical Genetics Service (CGS). Here we assess the clinical impact. At the time of data collection, the NWGLH had analysed 180 FFPE tissue samples from deceased affected individuals: 134 from breast and/or ovarian cancer cases for germline variants in the BRCA1/BRCA2 genes and 46 from colorectal, gastric, ovarian and endometrial cancer cases for germline variants in a panel of 13 genes implicated in inherited colorectal cancer and gastric cancer conditions. Successful analysis was achieved in 140/180 cases (78%). In total, 29 germline pathogenic/likely pathogenic variants were identified in autosomal dominant cancer predisposition genes where the gene was pertinent to the cancer family history (including BRCA1/BRCA2, the mismatch-repair genes and APC). Of the 180 cases, the impact of the result on clinical management of unaffected relatives was known in 143 cases. Of these, the results in 54 cases (38%) directly impacted the clinical management of relatives seen by the CGS. This included changes to risk assessments, screening recommendations and the availability of predictive genetic testing to unaffected relatives. Our data demonstrate how FFPE testing in deceased relatives is an accurate and informative tool in the clinical management of patients referred to the CGS.
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页码:861 / 871
页数:10
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