Damiola Francesca, Schultz Inès, Barjhoux Laure, Sornin Valérie, Dondon Marie-Gabrielle, Eon-Marchais Séverine, Marcou Morgane, Caron Olivier, Gauthier-Villars Marion, de Pauw Antoine, Luporsi Elisabeth, Berthet Pascaline, Delnatte Capucine, Bonadona Valérie, Maugard Christine, Pujol Pascal, Lasset Christine, Longy Michel, Bignon Yves-Jean, Fricker Jean-Pierre, Andrieu Nadine, Sinilnikova Olga M, Stoppa-Lyonnet Dominique, Mazoyer Sylvie, Muller Danièle
"Genetics of Breast Cancer" Team, Cancer Research Centre of Lyon, CNRS UMR5286/Inserm U1052/Université Lyon 1, Centre Léon Bérard, Lyon, France.
Unité d'Oncologie Génétique, Centre Paul Strauss, Strasbourg, France.
Breast Cancer Res Treat. 2015 Dec;154(3):463-71. doi: 10.1007/s10549-015-3625-7. Epub 2015 Nov 12.
Several population-based and family-based studies have demonstrated that germline mutations of the PALB2 gene (Partner and Localizer of BRCA2) are associated with an increased risk of breast cancer. Distinct mutation frequencies and spectrums have been described depending on the population studied. Here we describe the first complete PALB2 coding sequence screening in the French population. We screened the complete coding sequence and intron-exon boundaries of PALB2, using the EMMA technique, to assess the contribution of pathogenic mutations in a set of 835 familial breast cancer cases and 662 unrelated controls from the French national study GENESIS and the Paul Strauss Cancer Centre, all previously tested negative for BRCA1 and BRCA2 pathogenic mutations. Our analysis revealed the presence of four novel deleterious mutations: c.1186insT, c.1857delT and c.2850delC in three cases, c.3418dupT in one control. In addition, we identified two in-frame insertion/deletion, 19 missense substitutions (two of them predicted as pathogenic), 9 synonymous variants, 28 variants located in introns and 2 in UTRs, as well as frequent variants. Truncating PALB2 mutations were found in 0.36% of familial breast cancer cases, a frequency lower than the one detected in comparable studies in other populations (0.73-3.40%). This suggests a small but significant contribution of PALB2 mutations to the breast cancer susceptibility in the French population.
多项基于人群和基于家族的研究表明,PALB2基因(BRCA2的伙伴和定位蛋白)的种系突变与乳腺癌风险增加相关。根据所研究的人群,已描述了不同的突变频率和谱。在此,我们描述了法国人群中首次对PALB2完整编码序列的筛查。我们使用EMMA技术筛查了PALB2的完整编码序列和内含子-外显子边界,以评估在来自法国国家研究GENESIS和保罗·施特劳斯癌症中心的835例家族性乳腺癌病例和662例无关对照中,致病性突变的贡献,所有这些病例和对照之前BRCA1和BRCA2致病性突变检测均为阴性。我们的分析揭示了四个新的有害突变:三例中的c.1186insT、c.1857delT和c.2850delC,一例对照中的c.3418dupT。此外,我们鉴定出两个框内插入/缺失、19个错义替换(其中两个预测为致病性)、9个同义变体、28个位于内含子中的变体和2个位于非翻译区的变体,以及常见变体。在0.36%的家族性乳腺癌病例中发现了截短的PALB2突变,该频率低于在其他人群的类似研究中检测到的频率(0.73 - 3.40%)。这表明PALB2突变对法国人群乳腺癌易感性有微小但显著的贡献。
