Rios-Hoyo Alejandro, Xiong Kaitlyn, Dai Jiawei, Yau Christina, Marczyk Michal, Garcia-Milian Rolando, Wolf Denise M, Huppert Laura A, Nanda Rita, Hirst Gillian L, Cobain Erin F, van 't Veer Laura J, Esserman Laura J, Pusztai Lajos
Yale Cancer Center, Yale School of Medicine, New Haven, Connecticut.
Yale School of Medicine, New Haven, Connecticut.
Clin Cancer Res. 2025 Jan 17;31(2):403-413. doi: 10.1158/1078-0432.CCR-24-1553.
The MammaPrint (MP) prognostic assay categorizes breast cancers into high- and low-risk subgroups, and the high-risk group can be further subdivided into high-1 (MP-H1), and very high-risk high-2 (MP-H2). The aim of this analysis was to assess clinical and molecular differences between the hormone receptor-positive (HR+)/HER2-negative MP-H1, -H2, and triple-negative (TN) MP-H1 and -H2 cancers.
Pretreatment gene expression data from 742 HER2-negative breast cancers enrolled in the I-SPY2 neoadjuvant trial were used. Prognostic risk categories were assigned using the MP assay. Transcriptional similarities across the four receptor and prognostic groups were assessed using principal component analyses and by identifying differentially expressed genes. We also examined pathologic complete response rates and event-free survivals by risk group.
Principal component analysis showed that HR+/MP-H2 tumors clustered with TN/MP-H2 cancers. Only 125 genes showed differential expression between the HR+/MP-H2 and TN/MP-H2 cancers, whereas 1,465 genes were differentially expressed between HR+/MP-H2 and -H1. Gene set analysis revealed similarly high expression of cell cycle, DNA repair, and immune infiltration-related pathways in HR+/MP-H2 and TN/MP-H2 cancers. HR+/MP-H2 cancers also showed low estrogen receptor-related gene expression. Pathologic complete response rates were similarly high in TN/MP-H2 and HR+/MP-H2 cancers (42% vs. 30.5%; P = 0.11), and MP-H2 cancers with residual cancer had similarly poor event-free survival regardless of estrogen receptor status.
In conclusion, HR+/MP-H2 cancers closely resemble TN breast cancers in transcriptional and clinical features and benefit from similar treatment strategies.
MammaPrint(MP)预后检测将乳腺癌分为高风险和低风险亚组,高风险组可进一步细分为高风险1(MP-H1)和极高风险高风险2(MP-H2)。本分析的目的是评估激素受体阳性(HR+)/人表皮生长因子受体2阴性(HER2-)的MP-H1、-H2癌症与三阴性(TN)的MP-H1和-H2癌症之间的临床和分子差异。
使用了I-SPY2新辅助试验中纳入的742例HER2阴性乳腺癌的治疗前基因表达数据。使用MP检测确定预后风险类别。通过主成分分析和识别差异表达基因来评估四个受体和预后组之间的转录相似性。我们还按风险组检查了病理完全缓解率和无事件生存率。
主成分分析表明,HR+/MP-H2肿瘤与TN/MP-H2癌症聚集在一起。HR+/MP-H2和TN/MP-H2癌症之间只有125个基因表现出差异表达,而HR+/MP-H2和-H1之间有1465个基因差异表达。基因集分析显示,HR+/MP-H2和TN/MP-H2癌症中细胞周期、DNA修复和免疫浸润相关通路的表达同样高。HR+/MP-H2癌症还显示雌激素受体相关基因表达较低。TN/MP-H2和HR+/MP-H2癌症的病理完全缓解率同样高(42%对30.5%;P = 0.11),无论雌激素受体状态如何,有残留癌的MP-H2癌症的无事件生存率同样较差。
总之,HR+/MP-H2癌症在转录和临床特征上与TN乳腺癌非常相似,并受益于相似的治疗策略。
