Abstract

Simple SummaryGenotyping of BRCA genes is required for treatment with PARP inhibitors. Purposing to address treatment needs and familial cancer risk, the aim of our study was to introduce the most appropriate testing workflow in epithelial ovarian cancer patients (EOC) using germline and tumor genotyping of BRCA and other hereditary breast and/or ovarian cancer (HBOC) susceptibility genes. In consecutive patients with advanced non-mucinous EOC, who responded to platinum-based chemotherapy, germline and tumor genotyping were performed using Illumina’s next generation sequencing (NGS) panels. Sensitivity of tumor genotyping for detection of germline pathogenic/likely pathogenic variants (PV/LPV) was 96.2% for BRCA and 93.3% for HBOC genes. With germline genotyping-only strategy, 58.8% of HBOC PV/LPV and 68.4% of BRCA PV/LPV were detected. By tumor genotyping-only, 96.1% of HBOC PV/LPV and 97.4% of BRCA PV/LPV were detected. Tumor genotyping first followed by germline genotyping detects nearly all germline and somatic PV/LPV in the shortest time.Detection of germline and somatic pathogenic/likely pathogenic variants (PV/LPV) in BRCA genes is at the moment a prerequisite for use of PARP inhibitors in different treatment settings of different tumors. The aim of our study was to determine the most appropriate testing workflow in epithelial ovarian cancer (EOC) patients using germline and tumor genotyping of BRCA and other hereditary breast and/or ovarian cancer (HBOC) susceptibility genes. Consecutive patients with advanced non-mucinous EOC, who responded to platinum-based chemotherapy, were included in the study. DNA extracted from blood and FFPE tumor tissue were genotyped using NGS panels TruSightCancer/Hereditary and TruSight Tumor 170. Among 170 EOC patients, 21.8% had BRCA germline or somatic PV/LPV, and additionally 6.4% had PV/LPV in other HBOC genes. Sensitivity of tumor genotyping for detection of germline PV/LPV was 96.2% for BRCA genes and 93.3% for HBOC genes. With germline genotyping-only strategy, 58.8% of HBOC PV/LPV and 68.4% of BRCA PV/LPV were detected. By tumor genotyping-only strategy, 96.1% of HBOC PV/LPV and 97.4% of BRCA PV/LPV were detected. Genotyping of tumor first, followed by germline genotyping seems to be a reasonable approach for detection of PV/LPV in breast and/or ovarian cancer susceptibility genes in non-mucinous EOC patients.

Highlights

  • Ovarian cancer (OC) is the sixth leading cause of cancer death among Slovene women, according to the data from the Cancer Registry of Republic of Slovenia

  • The aim of our study was to determine the most appropriate testing workflow in epithelial ovarian cancer (EOC) patients using germline and tumor genotyping of BRCA and other hereditary breast and/or ovarian cancer (HBOC) susceptibility genes

  • In aforementioned subsequent studies reported percentage of somatic PV/LPV in BRCA genes ranged from 20% to 46% of all BRCA PV/LPV detected in EOC patients [6,7]

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Summary

Introduction

Ovarian cancer (OC) is the sixth leading cause of cancer death among Slovene women, according to the data from the Cancer Registry of Republic of Slovenia. Among epithelial ovarian cancer (EOC) tumors, high-grade serous carcinomas (HGSC) are highly aggressive, resulting in poor overall prognosis. 95% of HGSC tumors harbor TP53 pathogenic/likely pathogenic variants (PV/LPV) and more than 50% display homologous recombination deficiency [4,5]. According to early reports from the Cancer Genome Atlas data (TCGA), 20% of HGSC harbor a PV/LPV in the BRCA1 or BRCA2 gene, of which 17% are germline and 3% are somatic PV/LPV [4]. In aforementioned subsequent studies reported percentage of somatic PV/LPV in BRCA genes ranged from 20% to 46% of all BRCA PV/LPV detected in EOC patients [6,7]. Pathogenic/likely pathogenic variants in BRCA1 and BRCA2 genes were reported in endometroid and clear cell ovarian carcinoma in 15% (4/26) and 10% (2/19), respectively [5,8]

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