Oncogenetics Group, Vall d'Hebron Institute of Oncology-VHIO, Lab 2.02A, CELLEX CENTER, c/Natzaret, 115-117, 08035, Barcelona, Catalonia, Spain.
High Risk and Cancer Prevention Group, VHIO, Barcelona, Spain.
J Cancer Res Clin Oncol. 2018 Dec;144(12):2495-2513. doi: 10.1007/s00432-018-2763-9. Epub 2018 Oct 10.
Few and small studies have been reported about multigene testing usage by massively parallel sequencing in European cancer families. There is an open debate about what genes should be tested, and the actionability of some included genes is under research.
We investigated a panel of 34 known high/moderate-risk cancer genes, including 16 related to breast or ovarian cancer (BC/OC) genes, and 63 candidate genes to BC/OC in 192 clinically suspicious of hereditary breast/ovarian cancer (HBOC) Spanish families without pathogenic variants in BRCA1 or BRCA2 (BRCA1/2).
We identified 16 patients who carried a high- or moderate-risk pathogenic variant in eight genes: 4 PALB2, 3 ATM, 2 RAD51D, 2 TP53, 2 APC, 1 BRIP1, 1 PTEN and 1 PMS2. These findings led to increased surveillance or prevention options in 12 patients and predictive testing in their family members. We detected 383 unique variants of uncertain significance in known cancer genes, of which 35 were prioritized in silico. Eighteen loss-of-function variants were detected in candidate BC/OC genes in 17 patients (1 BARD1, 1 ERCC3, 1 ERCC5, 2 FANCE, 1 FANCI, 2 FANCL, 1 FANCM, 1 MCPH1, 1 PPM1D, 2 RBBP8, 3 RECQL4 and 1 with SLX4 and XRCC2), three of which also carry pathogenic variants in known cancer genes.
Eight percent of the BRCA1/2 negative patients carry pathogenic variants in other actionable genes. The multigene panel usage improves the diagnostic yield in HBOC testing and it is an effective tool to identify potentially new candidate genes.
关于欧洲癌症家族中使用大规模平行测序进行多基因检测的研究很少且规模较小。关于应该检测哪些基因存在争议,一些包含的基因的可操作性正在研究中。
我们研究了一个由 34 个已知的高/中风险癌症基因组成的小组,其中包括 16 个与乳腺癌或卵巢癌(BC/OC)相关的基因,以及 63 个候选基因用于 BC/OC,共涉及 192 个临床怀疑为遗传性乳腺癌/卵巢癌(HBOC)的西班牙家族,但 BRCA1 或 BRCA2(BRCA1/2)中没有致病性变异。
我们在 8 个基因中发现了 16 名患者携带高风险或中风险的致病性变异:4 个 PALB2、3 个 ATM、2 个 RAD51D、2 个 TP53、2 个 APC、1 个 BRIP1、1 个 PTEN 和 1 个 PMS2。这些发现导致 12 名患者增加了监测或预防选择,并对其家庭成员进行了预测性检测。我们在已知的癌症基因中检测到 383 个具有不确定意义的独特变体,其中 35 个变体在计算机上进行了优先级排序。在 17 名患者的候选 BC/OC 基因中检测到 18 个失活变体(1 个 BARD1、1 个 ERCC3、1 个 ERCC5、2 个 FANCE、1 个 FANCI、2 个 FANCL、1 个 FANCM、1 个 MCPH1、1 个 PPM1D、2 个 RBBP8、3 个 RECQL4 和 1 个带有 SLX4 和 XRCC2),其中 3 个基因也携带已知癌症基因的致病性变异。
8%的 BRCA1/2 阴性患者携带其他可操作基因的致病性变异。多基因检测面板的使用提高了 HBOC 检测的诊断率,是识别潜在新候选基因的有效工具。
