共识分子亚型和分子标志物与转移性结直肠癌患者临床结局的关联:LUME-Colon 1 的生物标志物分析。
Association of Consensus Molecular Subtypes and Molecular Markers With Clinical Outcomes in Patients With Metastatic Colorectal Cancer: Biomarker Analyses From LUME-Colon 1.
机构信息
University of Southern California Norris Comprehensive Cancer Center, Los Angeles, CA.
Vall d'Hebron University Hospital and Institute of Oncology (VHIO), Universitat Autònoma de Barcelona, Barcelona, Spain.
出版信息
Clin Colorectal Cancer. 2021 Mar;20(1):84-95.e8. doi: 10.1016/j.clcc.2020.09.003. Epub 2020 Sep 15.
INTRODUCTION
LUME-Colon 1 (NCT02149108) was a global, placebo-controlled phase III study of nintedanib in advanced colorectal cancer (CRC). Pre-specified biomarker analyses investigated the association of CRC consensus molecular subtypes (CMS) and tumor genomic and circulating biomarkers with clinical outcomes.
MATERIALS AND METHODS
Archival tumor tissue, cell-free DNA (cfDNA), and plasma samples were collected for genomic, transcriptomic, and proteomic analyses to investigate potential associations between CRC CMS and other biomarkers with nintedanib response and clinical outcomes.
RESULTS
Of the 765 treated patients, 735, 245, and 192 patient samples were analyzed in the circulating protein, tumor tissue, and cfDNA datasets, respectively. Patients were classified as CMS1 (1.7%), CMS2 (27.7%), CMS3 (0.9%), CMS4 (51.5%), or unclassified (18.2%). Unclassified/mixed CMS was associated with longer overall survival (OS) with nintedanib vs. CMS2 or CMS4 (interaction P-value = .0086); no association was observed for CMS4. Gene expression-based pathway analysis revealed an association between vascular endothelial growth factor-related signaling and OS for nintedanib (P = .0498). The most frequently detected somatic mutations were APC (72.0% [tumor tissue] vs. 56.8% [cfDNA]), TP53 (47.1% vs. 34.9%), KRAS (40.8% vs. 28.6%), and PIK3CA (16.6% vs. 11.5%); concordance rates were > 80%. Median OS differences were observed for APC and TP53 mutations vs. wild-type in cfDNA, indicating a potential prognostic value. Circulating ANG-2, CA-9, CEACAM1, collagen-IV, IGFBP-1, ICAM-1, IL-8, and uPAR were potentially prognostic for both OS and progression-free survival.
CONCLUSION
We demonstrated the feasibility of large-scale biomarker analyses and CMS classification within a global clinical trial, and identified signals suggesting a potential for greater nintedanib treatment response in the unclassified/mixed CMS subgroup, despite these tumors showing heterogeneous patterns of CMS mixtures. Our results revealed a high degree of concordance in somatic mutations between tumor tissue and cfDNA. Associations with prognosis for cfDNA somatic mutations, as well as several protein-based biomarkers, may warrant further investigation in future trials.
简介
LUME-Colon 1(NCT02149108)是一项全球、安慰剂对照的 III 期尼替西农治疗晚期结直肠癌(CRC)的研究。预先指定的生物标志物分析研究了 CRC 共识分子亚型(CMS)和肿瘤基因组及循环生物标志物与临床结局的关系。
材料与方法
收集存档的肿瘤组织、无细胞 DNA(cfDNA)和血浆样本,进行基因组、转录组和蛋白质组分析,以研究 CRC CMS 与其他生物标志物与尼替西农反应和临床结局之间的潜在关联。
结果
在 765 名接受治疗的患者中,分别对循环蛋白、肿瘤组织和 cfDNA 数据集中的 735、245 和 192 名患者样本进行了分析。患者被分类为 CMS1(1.7%)、CMS2(27.7%)、CMS3(0.9%)、CMS4(51.5%)或未分类(18.2%)。未分类/混合 CMS 与尼替西农的总生存期(OS)延长相关,与 CMS2 或 CMS4 相比(交互 P 值=.0086);未观察到 CMS4 的相关性。基于基因表达的途径分析显示,血管内皮生长因子相关信号与尼替西农的 OS 相关(P=.0498)。最常检测到的体细胞突变是 APC(72.0%[肿瘤组织]比 56.8%[cfDNA])、TP53(47.1%比 34.9%)、KRAS(40.8%比 28.6%)和 PIK3CA(16.6%比 11.5%);一致性率>80%。在 cfDNA 中观察到 APC 和 TP53 突变与野生型的中位 OS 差异,表明其具有潜在的预后价值。循环 ANG-2、CA-9、CEACAM1、胶原-IV、IGFBP-1、ICAM-1、IL-8 和 uPAR 可能对 OS 和无进展生存期均具有预后价值。
结论
我们在一项全球临床试验中证明了大规模生物标志物分析和 CMS 分类的可行性,并发现了信号,表明尽管这些肿瘤显示出 CMS 混合的异质性模式,但未分类/混合 CMS 亚组中尼替西农治疗反应的潜力更大。我们的结果显示,肿瘤组织和 cfDNA 之间的体细胞突变具有高度一致性。cfDNA 体细胞突变以及几种基于蛋白质的生物标志物与预后的相关性可能需要在未来的试验中进一步研究。
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