Identification of a novel pathogenic variant in PALB2 and BARD1 genes by a multigene sequencing panel in triple negative breast cancer in Morocco.

Journal of Genomics Pub Date : 2021-09-18 eCollection Date: 2021-01-01 DOI:10.7150/jgen.61713

Abdelilah Laraqui, Mathias Cavaillé, Nancy Uhrhammer, Oubaida ElBiad, Yannick Bidet, Hicham El Rhaffouli, Hicham El Anaz, Driss Moussaoui Rahali, Jaouad Kouach, Khaled Guelzim, Bouabid Badaoui, Abderrahman AlBouzidi, Mohammed Oukabli, Rachid Tanz, Yasser Sbitti, Mohammed Ichou, Khaled Ennibi, Yassine Sekhsokh, Yves-Jean Bignon

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引用次数: 4

Abstract

Pathogenic variants (PVs) in BRCA genes have been mainly associated with an increasing risk of triple negative breast cancer (TNBC). The contribution of PVs in non-BRCA genes to TNBC seems likely since the processing of homologous recombination repair of double-strand DNA breaks involves several genes. Here, we investigate the susceptibility of genetic variation of the BRCA and non-BRCA genes in 30 early-onset Moroccan women with TNBC. Methods: Targeted capture-based next generation sequencing (NGS) method was performed with a multigene panel testing (MGPT) for variant screening. Panel sequencing was performed with genes involved in hereditary predisposition to cancer and candidate genes whose involvement remains unclear using Illumina MiSeq platform. Interpretation was conducted by following the American College of Medical Genetics and Genomics-Association for Molecular Pathology (ACMG-AMP) criteria. Results: PVs were identified in 20% (6/30) of patients with TNBC. Of these, 16.7% (5/30) carried a BRCA PV [10% (3/30) in BRCA1, 6.7% (2/30) in BRCA2] and 6.6% (2/30) carried a non-BRCA PV. The identified PVs in BRCA genes (BRCA1 c.798_799delTT, BRCA1 c.3279delC, BRCA2 c.1310_1313del, and BRCA2 c.1658T>G) have been reported before and were classified as pathogenic. The identified founder PVs BRCA1 c.798_799del and BRCA2 c.1310_1313delAAGA represented 10% (3/30). Our MGPT allowed identification of several sequence variations in most investigated genes, among which we found novel truncating variations in PALB2 and BARD1 genes. The PALB2 c.3290dup and BARD1 c.1333G>T variants are classified as pathogenic. We also identified 42 variants of unknown/uncertain significance (VUS) in 70% (21/30) of patients with TNBC, including 50% (21/42) missense variants. The highest VUS rate was observed in ATM (13%, 4/30). Additionally, 35.7% (15/42) variants initially well-known as benign, likely benign or conflicting interpretations of pathogenicity have been reclassified as VUS according to ACMG-AMP. Conclusions: PALB2 and BARD1 along with BRCA genetic screening could be helpful for a larger proportion of early-onset TNBC in Morocco.

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通过多基因测序小组在摩洛哥三阴性乳腺癌中鉴定一种新的PALB2和BARD1基因致病变异。

BRCA基因的致病性变异（PV）主要与癌症（TNBC）三阴性风险的增加有关。非BRCA基因中的PV对TNBC的贡献似乎很可能，因为双链DNA断裂的同源重组修复过程涉及几个基因。在这里，我们研究了30名早发性摩洛哥TNBC妇女BRCA和非BRCA基因遗传变异的易感性。方法：基于靶向捕获的下一代测序（NGS）方法采用多基因面板试验（MGPT）进行变异筛查。使用Illumina MiSeq平台对参与癌症遗传易感性的基因和参与尚不清楚的候选基因进行面板测序。根据美国医学遗传学和基因组学学会分子病理学（ACMG-AMP）标准进行解释。结果：20%（6/30）的TNBC患者中发现PV。其中，16.7%（5/30）携带BRCA PV[10%（3/30）BRCA1，6.7%（2/30）BRCA2]，6.6%（2/30）携带非BRCA PV。BRCA基因中已鉴定的PV（BRCA1 c.798_799delTT、BRCA1 c.3279delC、BRCA2 c.1310_11313del和BRCA2 c.1658T>G）以前已有报道，并被归类为致病性。已确定的创始人PV BRCA1 c.798_799del和BRCA2 c.1310_11313delAAGA占10%（3/30）。我们的MGPT能够鉴定大多数研究基因中的几个序列变异，其中我们在PALB2和BARD1基因中发现了新的截短变异。PALB2 c.3290dup和BARD1 c.1333G>T变体被归类为致病性变体。我们还在70%（21/30）的TNBC患者中发现了42种意义未知/不确定的变异（VUS），其中包括50%（21/42）的错义变异。在ATM中观察到最高的VUS率（13%，4/30）。此外，根据ACMG-AMP，35.7%（15/42）最初被认为是良性、可能是良性或相互矛盾的致病性解释的变体已被重新归类为VUS。结论：PALB2和BARD1以及BRCA基因筛查可能有助于摩洛哥更大比例的早发性TNBC。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Journal of Genomics

自引率

0.00%

发文量

审稿时长

12 weeks

期刊介绍： Journal of Genomics publishes papers of high quality in all areas of gene, genetics, genomics, proteomics, metabolomics, DNA/RNA, computational biology, bioinformatics, and other relevant areas of research and application. Articles published by the journal are rigorously peer-reviewed. Types of articles include: Research paper, Short research communication, Review or mini-reviews, Commentary, Database, Software.