Germline mutations of breast cancer susceptibility genes through expanded genetic analysis in unselected Colombian patients.

IF 3.8 3区 医学 Q2 GENETICS & HEREDITY Human Genomics Pub Date : 2024-06-18 DOI:10.1186/s40246-024-00623-7
Diana Carolina Sierra-Díaz, Adrien Morel, Dora Janeth Fonseca-Mendoza, Nora Contreras Bravo, Nicolas Molano-Gonzalez, Mariana Borras, Isabel Munevar, Mauricio Lema, Henry Idrobo, Daniela Trujillo, Norma Serrano, Ana Isabel Orduz, Diego Lopera, Jaime González, Gustavo Rojas, Paula Londono-De Los Ríos, Ray Manneh, Rodrigo Cabrera, Wilson Rubiano, Jairo de la Peña, María Catalina Quintero, William Mantilla, Carlos M Restrepo
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Abstract

Background: In Colombia and worldwide, breast cancer (BC) is the most frequently diagnosed neoplasia and the leading cause of death from cancer among women. Studies predominantly involve hereditary and familial cases, demonstrating a gap in the literature regarding the identification of germline mutations in unselected patients from Latin-America. Identification of pathogenic/likely pathogenic (P/LP) variants is important for shaping national genetic analysis policies, genetic counseling, and early detection strategies. The present study included 400 women with unselected breast cancer (BC), in whom we analyzed ten genes, using Whole Exome Sequencing (WES), know to confer risk for BC, with the aim of determining the genomic profile of previously unreported P/LP variants in the affected population. Additionally, Multiplex Ligation-dependent Probe Amplification (MLPA) was performed to identify Large Genomic Rearrangements (LGRs) in the BRCA1/2 genes. To ascertain the functional impact of a recurrent intronic variant (ATM c.5496 + 2_5496 + 5delTAAG), a minigene assay was conducted.

Results: We ascertained the frequency of P/LP germline variants in BRCA2 (2.5%), ATM (1.25%), BRCA1 (0.75%), PALB2 (0.50%), CHEK2 (0.50%), BARD1 (0.25%), and RAD51D (0.25%) genes in the population of study. P/LP variants account for 6% of the total population analyzed. No LGRs were detected in our study. We identified 1.75% of recurrent variants in BRCA2 and ATM genes. One of them corresponds to the ATM c.5496 + 2_5496 + 5delTAAG. Functional validation of this variant demonstrated a splicing alteration probably modifying the Pincer domain and subsequent protein structure.

Conclusion: This study described for the first time the genomic profile of ten risk genes in Colombian women with unselected BC. Our findings underscore the significance of population-based research, advocating the consideration of molecular testing in all women with cancer.

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通过对未入选的哥伦比亚患者进行扩展基因分析,发现乳腺癌易感基因的种系突变。
背景:在哥伦比亚和全世界,乳腺癌(BC)是最常见的肿瘤,也是女性死于癌症的主要原因。研究主要涉及遗传性和家族性病例,这表明在拉丁美洲未经选择的患者的种系突变鉴定方面存在文献空白。致病/可能致病(P/LP)变异的鉴定对于制定国家遗传分析政策、遗传咨询和早期检测策略非常重要。本研究纳入了 400 名未经筛选的乳腺癌(BC)女性患者,我们利用全外显子组测序(WES)技术分析了其中 10 个已知具有 BC 风险的基因,目的是确定受影响人群中以前未报告的 P/LP 变异基因组概况。此外,还进行了多重连接依赖性探针扩增(MLPA),以确定 BRCA1/2 基因中的大基因组重排(LGR)。为了确定复发性内含子变异(ATM c.5496 + 2_5496 + 5delTAAG)的功能影响,进行了一项微型基因检测:我们确定了研究人群中 BRCA2(2.5%)、ATM(1.25%)、BRCA1(0.75%)、PALB2(0.50%)、CHEK2(0.50%)、BARD1(0.25%)和 RAD51D(0.25%)基因的 P/LP 种系变异频率。P/LP变异占分析人群总数的6%。在我们的研究中没有发现 LGR。我们在 BRCA2 和 ATM 基因中发现了 1.75% 的复发性变异。其中一个对应于 ATM c.5496 + 2_5496 + 5delTAAG。该变异的功能验证表明,剪接改变可能会改变 Pincer 结构域和随后的蛋白质结构:本研究首次描述了哥伦比亚女性非选择性 BC 患者中 10 个风险基因的基因组概况。我们的研究结果强调了基于人群的研究的重要性,提倡考虑对所有癌症妇女进行分子检测。
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来源期刊
Human Genomics
Human Genomics GENETICS & HEREDITY-
CiteScore
6.00
自引率
2.20%
发文量
55
审稿时长
11 weeks
期刊介绍: Human Genomics is a peer-reviewed, open access, online journal that focuses on the application of genomic analysis in all aspects of human health and disease, as well as genomic analysis of drug efficacy and safety, and comparative genomics. Topics covered by the journal include, but are not limited to: pharmacogenomics, genome-wide association studies, genome-wide sequencing, exome sequencing, next-generation deep-sequencing, functional genomics, epigenomics, translational genomics, expression profiling, proteomics, bioinformatics, animal models, statistical genetics, genetic epidemiology, human population genetics and comparative genomics.
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