Solano Angela Rosaria, Cardoso Florencia Cecilia, Romano Vanesa, Perazzo Florencia, Bas Carlos, Recondo Gonzalo, Santillan Francisco Bernardo, Gonzalez Eduardo, Abalo Eduardo, Viniegra María, Michel José Davalos, Nuñez Lina María, Noblia Cristina Maria, Mc Lean Ignacio, Canton Enrique Diaz, Chacon Reinaldo Daniel, Cortese Gustavo, Varela Eduardo Beccar, Greco Martín, Barrientos María Laura, Avila Silvia Adela, Vuotto Hector Daniel, Lorusso Antonio, Podesta Ernesto Jorge, Mando Oscar Gaspar
Genotipificación y Cáncer Hereditario, Centro de Educación Médicae Investigaciones Clínicas "Norberto Quirno" (CEMIC), Buenos Aires, Argentina.
Instituto de Investigaciones Bioquímicas (INBIOMED), Facultad de Medicina, Universidad de Buenos Aires-CONICET, Buenos Aires, Argentina.
Oncotarget. 2016 Jul 24;8(36):60487-60495. doi: 10.18632/oncotarget.10814. eCollection 2017 Sep 1.
mutations in Latin America are scarcely documented and in serious need of knowledge about the spectrum of BRCA pathogenic variants, information which may alter clinical practice and subsequently improve patient outcome. In addition, the search for data on testing policies in different regions constitutes a fundamental strength for the present study, which analyzes gene sequences and large rearrangements in 940 probands with familial and/or personal history of breast/ovary cancer (BOC). In non-mutated DNA samples, Multiplex Ligation-dependent Probe Amplification assays (MLPA) were used for the analysis of large rearrangements. Our studies detected 179 deleterious mutations out of 940 (19.04%) probands, including 5 large rearrangements and 22 novel mutations. The recurrent mutations accounted for 15.08% of the total and only 2.87% of the probands analyzed, very different from a Hispanic panel previously described.
a) this first comprehensive description of the spectrum in BRCA1/2 sheds light on the low frequency of recurrent mutations; b) this information is key in clinical practice to select adequate sequencing studies in our population, subsequently improve patient outcome and prevent damage associated to false normal reports resulting from the use of invalid population panels; c) panels of mutations from other populations should be cautiously validated before imported, even those of apparently similar origin, a concept to be considered beyond significance in Argentina.
拉丁美洲的突变情况鲜有记录,亟需了解BRCA致病变异谱,这些信息可能会改变临床实践并进而改善患者预后。此外,查找不同地区检测政策的数据是本研究的一项重要优势,该研究分析了940名有乳腺癌/卵巢癌(BOC)家族史和/或个人史的先证者的基因序列和大片段重排。对于未发生突变的DNA样本,采用多重连接依赖探针扩增法(MLPA)分析大片段重排。我们的研究在940名先证者中检测到179个有害突变(19.04%),包括5个大片段重排和22个新突变。复发突变占总数的15.08%,仅占所分析先证者的2.87%,与先前描述的西班牙裔样本差异很大。
a)对BRCA1/2变异谱的首次全面描述揭示了复发突变的低频率;b)该信息在临床实践中对于选择适合我们人群的测序研究至关重要,进而改善患者预后,并防止因使用无效人群样本导致假正常报告相关的损害;c)在引入其他人群的突变样本之前,应谨慎验证,即使是那些明显来源相似的样本,这一概念在阿根廷具有重要意义。
