Franco Idalid, Alshalalfa Mohammed, Hernandez Alexandra, Mahal Brandon A, Nguyen Tiffany, Wang Lora, Punglia Rinaa, Swami Nishwant, Goel Neha
Department of Radiation Oncology, Brigham and Women's Hospital/Dana-Farber Cancer Institute, Boston, MA, USA.
Department of Radiation Oncology, University of Miami Miller School of Medicine, Miami, FL, USA.
Ann Surg Oncol. 2023 Nov;30(12):7569-7578. doi: 10.1245/s10434-023-14080-4. Epub 2023 Aug 7.
Although breast cancer (BC) risk increases with age, BC in younger women is more aggressive with higher mortality compared with older women. We characterize the genomic landscape of BCs in younger women.
Clinicopathologic, molecular, and genomic differences across age groups (< 40 years, 40-60 years, > 60 years) in female BC patients were investigated in two large cohorts [AACR-GENIE8.1 (n = 11,594) and METABRIC (n = 2509)]. Cox-proportional regression analyzed the prognostic impact of age groups for disease-specific survival (DSS) and recurrence-free survival (RFS) in METABRIC and progression-free survival (PFS) in GENIE cohorts. Chi-squared test was used to assess statistical associations between genomic alterations and age groups.
Survival analysis showed that women < 40 years had shorter DSS [hazard ratio (HR): 1.52, p = 0.005], RFS (HR: 1.4, p = 0.006), and PFS (HR: 1.82, p = 0.0003) compared with women 40-60 years, and shorter RFS (HR: 1.5, p = 0.001) and PFS (HR: 2.95, p < 0.0001) compared with women > 60 years. Molecular subtypes in the METABRIC cohort showed women < 40 years were enriched with basal, and HER2+ subtypes, and less enriched with luminal A and B subtype (p < 0.0001). Characterization of genomic alterations in both cohorts demonstrated that BCs in women < 40 years were more enriched with TP53 mutations (FDR < 0.0001), BRCA1 mutations (FDR = 0.01), ERBB2 amplifications (FDR < 0.001), CDK12 amplifications (FDR < 0.001), and PPM1D amplifications (FDR < 0.001). In contrast, BCs in older women (> 60 years) were more enriched with PIK3CA, KMT2C, and CDH1 mutations (FDR < 0.0001).
BCs in young women are associated with shorter survival and more aggressive genomic features, including mutations in TP53 and BRCA1, and amplifications in ERBB2 and CDK12. These findings have the potential to impact clinical trial design and treatment.
尽管乳腺癌(BC)风险随年龄增长而增加,但与老年女性相比,年轻女性的乳腺癌更具侵袭性,死亡率更高。我们对年轻女性乳腺癌的基因组特征进行了描述。
在两个大型队列[AACR-GENIE8.1(n = 11,594)和METABRIC(n = 2509)]中,研究了女性乳腺癌患者不同年龄组(<40岁、40 - 60岁、>60岁)之间的临床病理、分子和基因组差异。Cox比例回归分析了年龄组对METABRIC队列中疾病特异性生存(DSS)和无复发生存(RFS)以及GENIE队列中无进展生存(PFS)的预后影响。卡方检验用于评估基因组改变与年龄组之间的统计学关联。
生存分析表明,与40 - 60岁的女性相比,<40岁的女性DSS更短[风险比(HR):1.52,p = 0.005]、RFS更短(HR:1.4,p = 0.006)和PFS更短(HR:1.82,p = 0.0003);与>60岁的女性相比,<40岁的女性RFS更短(HR:1.5,p = 0.001)和PFS更短(HR:2.95,p < 0.0001)。METABRIC队列中的分子亚型显示,<40岁的女性中基底型和HER2 +亚型富集,而管腔A型和B型亚型富集较少(p < 0.0001)。两个队列中基因组改变的特征表明,<40岁女性的乳腺癌中TP53突变(FDR < 0.0001)、BRCA1突变(FDR = 0.01)、ERBB2扩增(FDR < 0.001)、CDK12扩增(FDR < 0.001)和PPM1D扩增(FDR < 0.001)更为富集。相比之下,老年女性(>60岁)的乳腺癌中PIK3CA、KMT2C和CDH1突变更为富集(FDR < 0.0001)。
年轻女性的乳腺癌与较短的生存期和更具侵袭性的基因组特征相关,包括TP�3和BRCA1突变以及ERBB2和CDK۱۲扩增。这些发现有可能影响临床试验设计和治疗。
