Beltran-Bless Ana-Alicia, Pond Gregory R, Bayani Jane, Barker Sarah L, Spears Melanie, Mallon Elizabeth, Taylor Karen J, Hasenburg Annette, Markopoulos Christos, Dirix Luc, Meershoek-Klein Kranenbarg Elma, van de Velde Cornelis J H, Rea Daniel W, Vandermeer Lisa, Hilton John, Bartlett John M S, Clemons Mark
Division of Medical Oncology, Department of Medicine, The University of Ottawa, Ottawa, Canada.
Department of Oncology, McMaster University, Hamilton, Canada.
Breast. 2025 Jul 4;83:104528. doi: 10.1016/j.breast.2025.104528.
Few studies have compared the performance of gene-expression profiling tests (e.g. Oncotype-Dx) to clinico-pathologic risk calculators (e.g. PREDICT 2.1, INFLUENCE 2.0, and CTS5) or tools that combine both (e.g. RSClin) in patients with early breast cancer (EBC). A large trial dataset was used to evaluate the prognostic performance of different tests based on patient outcomes.
The TEAM pathology cohort accrued samples from 4736 postmenopausal hormone positive women with EBC, treated with either exemestane or tamoxifen followed by exemestane. Oncotype-Dx-trained risk scores were previously generated by gene-expression profiling. Patient data was used to calculate various recurrence scores. Analysis was restricted to the N0/N1 population and prognostic ability of selected risk tools was assessed using Cox regression analysis and Harrell's C-statistic.
Results were available for 2065 patients. There was low correlation between PREDICT 2.1 (r = -0.12), INFLUENCE 2.0 (r = 0.20), CTS5 (r = 0.16) with Oncotype-Dx-trained results. In N0 patients, RSClin had improved prognostic ability (C-statistic = 0.66) on DMFS compared to PREDICT 2.1 (0.60), INFLUENCE 2.0 (0.57), CTS-5 (0.62), and Oncotype-Dx (0.63).
Combining molecular and clinico-pathologic factors enhances prognostic information. However, the impact of this on actual patient management requires further prospective validation. The trial is registered with clinicaltrials.gov NCT00279448 and NCT00032136; with Netherlands Trial Register, number NTR 267; and the Ethics Commission Trial, number 27/2001.
很少有研究比较基因表达谱检测(如Oncotype-Dx)与临床病理风险计算器(如PREDICT 2.1、INFLUENCE 2.0和CTS5)或两者结合的工具(如RSClin)在早期乳腺癌(EBC)患者中的性能。一项大型试验数据集用于根据患者结局评估不同检测的预后性能。
TEAM病理学队列收集了4736名绝经后激素阳性EBC女性的样本,这些患者接受了依西美坦或他莫昔芬治疗,随后接受依西美坦治疗。之前通过基因表达谱生成了Oncotype-Dx训练的风险评分。患者数据用于计算各种复发评分。分析仅限于N0/N1人群,并使用Cox回归分析和Harrell's C统计量评估所选风险工具的预后能力。
2065名患者有结果。PREDICT 2.1(r = -0.12)、INFLUENCE 2.0(r = 0.20)、CTS5(r = 0.16)与Oncotype-Dx训练结果之间的相关性较低。在N0患者中،与PREDICT 2.1(0.60)、INFLUENCE 2.0(0.57)、CTS-5(0.62)和Oncotype-Dx(0.63)相比,RSClin在无远处转移生存期(DMFS)方面具有更好的预后能力(C统计量 = 0.66)。
结合分子和临床病理因素可增强预后信息。然而,这对实际患者管理的影响需要进一步的前瞻性验证。该试验已在clinicaltrials.gov上注册,编号为NCT00279448和NCT00032136;在荷兰试验注册中心,编号为NTR 267;以及伦理委员会试验,编号为27/2001。
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