Boscolo Bielo Luca, Guerini Rocco Elena, Crimini Edoardo, Repetto Matteo, Lombardi Mariano, Zanzottera Cristina, Aurilio Gaetano, Barberis Massimo, Belli Carmen, Zhan Yinxiu, Battaiotto Elena, Katrini Jalissa, Marsicano Renato, Zagami Paola, Taurelli Salimbeni Beatrice, Esposito Angela, Trapani Dario, Criscitiello Carmen, Fusco Nicola, Marra Antonio, Curigliano Giuseppe
Division of Early Drug Development for Innovative Therapies, European Institute of Oncology IRCCS, Via G. Ripamonti 435, 20141, Milan, Italy.
Department of Oncology and Hemato-Oncology, University of Milano, Milan, Italy.
Breast Cancer Res Treat. 2025 Feb;210(1):45-55. doi: 10.1007/s10549-024-07535-z. Epub 2024 Oct 30.
Comprehensive genomic profiling is becoming increasingly important in the management of patients with metastatic breast cancer (mBC). Real-world clinical outcomes from applying molecular tumor boards (MTBs) recommendations in this context remain limited. Accordingly, we conducted a retrospective, single-institution analysis to evaluate the clinical impact of discussing patients affected by mBC at the MTB.
Clinicogenomic data of patients affected by mBCs referred to the European Institute of Oncology MTB between August 2019 and December 2023 were reviewed. Genomic alterations were classified by ESCAT framework. Clinical outcomes of patients showing actionable alterations and receiving molecular-matched therapy (MMT) were compared to those receiving standard therapy (ST).
Ninety-six patients were included. Following MTB discussion, genetic counseling was recommended in 27% (n = 26) of patients, while additional molecular analyses were requested in 25% (n = 24) cases. Fifty-six patients (58%) displayed at least one actionable alteration. For patients with available follow-up (n = 50), 32 (64%) received MMTs and 18 (36%) ST. No differences in real-world progression-free survival (rwPFS) (4.07 months [95% CI 2.14-8.28] vs. 3.12 months [95% CI 1.51-NE], P = 0.8) and 12-month overall survival (OS) (58% [95%CI 43-78] vs. 57% [95%CI 34-97), P = 0.9) were observed between the MMT- and ST-group. Level I ESCAT alterations yielded longer rwPFS (5.82 months [95% CI 3.12-8.41]) compared to ESCAT II (2.14 months [95%CI 1.61-NE]) and ESCAT III (2.10 months [95% CI 2.04-NE]; P = 0.03). Twenty-four percent of patients showed a PFS2/PFS1 ratio > 1.3 from MMT.
Molecular tumor boards can provide additional treatment options for patients affected by mBC. Besides treatment recommendations, MTBs also have the utility to assess the validity of discussed genomic reports and to identify alterations worthy of genetic counseling.
全面基因组分析在转移性乳腺癌(mBC)患者的管理中变得越来越重要。在这种情况下应用分子肿瘤委员会(MTB)建议的真实世界临床结果仍然有限。因此,我们进行了一项回顾性单机构分析,以评估在MTB讨论mBC患者的临床影响。
回顾了2019年8月至2023年12月间转诊至欧洲肿瘤研究所MTB的mBC患者的临床基因组数据。基因组改变按ESCAT框架分类。将显示可操作改变并接受分子匹配治疗(MMT)的患者与接受标准治疗(ST)的患者的临床结果进行比较。
纳入96例患者。在MTB讨论后,27%(n = 26)的患者被建议进行遗传咨询,而25%(n = 24)的病例被要求进行额外的分子分析。56例患者(58%)显示至少一种可操作改变。对于有可用随访数据的患者(n = 50),32例(64%)接受MMT,18例(36%)接受ST。MMT组和ST组在真实世界无进展生存期(rwPFS)(4.07个月[95%CI 2.14 - 8.28] vs. 3.12个月[95%CI 1.51 - NE],P = 0.8)和12个月总生存期(OS)(58%[95%CI 43 - 78] vs. 57%[95%CI 34 - 97],P = 0.9)方面未观察到差异。与ESCAT II(2.14个月[95%CI 1.61 - NE])和ESCAT III(2.10个月[95%CI 2.04 - NE];P = 0.03)相比,I级ESCAT改变产生更长的rwPFS(5.82个月[95%CI 3.12 - 8.41])。24%的患者MMT后的PFS2/PFS1比值>1.3。
分子肿瘤委员会可为mBC患者提供额外的治疗选择。除了治疗建议外,MTB还有助于评估所讨论基因组报告的有效性,并识别值得进行遗传咨询的改变。
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