Agrawal Yash N, Fernández-Martínez Aranzazu, Gil-Gil Miguel, Zielinski Christoph, Ruiz-Borrego Manuel, Ciruelos Eva María, Muñoz Montserrat, Margelí Mireia, Bermejo Begoña, Antón Antonio, Kahan Zsuzsanna, Csöszi Tibor, Alonso-Romero José Luis, García-Saenz José Ángel, Sánchez-Rovira Pedro, Álvarez Elena, Chacón José Ignacio, González-Santiago Santiago, Rodríguez César A, Servitja Sonia, Pfefferle Adam D, Herranz Jesús, Liu Yuan, Carey Lisa A, Romero-Camarero Isabel, Caballero Rosalía, Guerrero-Zotano Ángel, Perou Charles M, Martín Miguel
Lineberger Comprehensive Cancer Center, University of North Carolina, Chapel Hill, NC.
Division of Oncology, Department of Medicine, School of Medicine, University of North Carolina at Chapel Hill, Chapel Hill, NC.
JCO Precis Oncol. 2025 Jul;9:e2400937. doi: 10.1200/PO-24-00937. Epub 2025 Jul 9.
For hormone receptor-positive/human epidermal growth factor receptor 2-negative (HR+/HER2-) metastatic breast cancer (MBC), first-line cyclin-dependent kinase 4/6 inhibitors (CDK4/6i) + endocrine therapy (ET) is the standard of care. They are also used after progression on first-line aromatase inhibitors (AIs), but some patients may respond better to chemotherapy-based options. We examined tumor features associated with survival from GEICAM/2013-02 PEARL, a phase III trial of palbociclib + ET versus capecitabine in AI-resistant HR+/HER2- MBC.
For 158 and 155 patients from each arm, 878 previously published gene expression signatures were derived using RNA sequencing on pretreatment tumor specimens, both primary and metastatic. Multivariable Cox models for progression-free survival (PFS) and overall survival (OS) were constructed with 16 preselected signatures related to proliferation, loss of retinoblastoma, and immune infiltration, and via Elastic Net using all signatures.
Significant PFS difference by PAM50 intrinsic subtype was observed with palbociclib + ET. Comparing treatment arms, luminal A subtype trended toward longer PFS with palbociclib + ET, and luminal B and nonluminal subtypes had significantly longer PFS with capecitabine. Three B-cell (B-lymphocyte)-associated signatures correlated with shorter OS with palbociclib + ET. The immune-activated Immune1 TCGA breast cancer signature had significant treatment arm interaction for OS. Elastic Net iteratively selected B-cell-associated signatures independently associated with shorter OS with palbociclib + ET.
PAM50 intrinsic subtype predicted PFS differences between palbociclib + ET and capecitabine. Lower B-cell-associated gene expression predicted longer OS with palbociclib + ET versus capecitabine. These features may help identify HR+/HER2- tumors resistant to further ET-based treatment with CDK4/6i.
对于激素受体阳性/人表皮生长因子受体2阴性(HR+/HER2-)转移性乳腺癌(MBC),一线细胞周期蛋白依赖性激酶4/6抑制剂(CDK4/6i)+内分泌治疗(ET)是标准治疗方案。它们也用于一线芳香化酶抑制剂(AI)治疗进展后,但有些患者可能对基于化疗的方案反应更好。我们在GEICAM/2013-02 PEARL试验中研究了与生存相关的肿瘤特征,该试验是一项关于帕博西尼+ET对比卡培他滨治疗AI耐药HR+/HER2- MBC的III期试验。
对每组158例和155例患者,使用RNA测序对预处理的原发性和转移性肿瘤标本得出878个先前发表的基因表达特征。构建无进展生存期(PFS)和总生存期(OS)的多变量Cox模型,模型纳入16个与增殖、视网膜母细胞瘤缺失和免疫浸润相关的预选特征,并通过弹性网络法纳入所有特征。
帕博西尼+ET治疗组中,PAM50内在亚型对PFS有显著差异。比较治疗组,腔面A型亚型接受帕博西尼+ET治疗时PFS有延长趋势,腔面B型和非腔面型亚型接受卡培他滨治疗时PFS显著延长。三个与B细胞(B淋巴细胞)相关的特征与帕博西尼+ET治疗的较短OS相关。免疫激活的Immune1 TCGA乳腺癌特征在OS方面有显著的治疗组交互作用。弹性网络法迭代选择出与帕博西尼+ET治疗的较短OS独立相关的B细胞相关特征。
PAM50内在亚型预测了帕博西尼+ET和卡培他滨之间的PFS差异。较低的B细胞相关基因表达预示着帕博西尼+ET对比卡培他滨治疗有更长的OS。这些特征可能有助于识别对基于CDK4/6i的进一步ET治疗耐药的HR+/HER2-肿瘤。
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