Thoracic Service, Department of Surgery, Memorial Sloan Kettering Cancer Center, New York, New York.
Center for Molecular Oncology, Memorial Sloan Kettering Cancer Center, New York, New York.
Clin Cancer Res. 2021 Jun 15;27(12):3491-3498. doi: 10.1158/1078-0432.CCR-20-4707. Epub 2021 Apr 1.
To delineate recurrent oncogenic driver alterations and dysregulated pathways in esophageal adenocarcinoma and to assess their prognostic value.
We analyzed a large cohort of patients with lower esophageal and junctional adenocarcinoma, prospectively sequenced by MSK-IMPACT with high-quality clinical annotation. Patients were subdivided according to treatment intent, curative versus palliative, which closely mirrored clinical staging. Genomic features, alterations, and pathways were examined for association with overall survival using Cox proportional hazard models, adjusted for relevant clinicopathologic factors knowable at the time of diagnosis.
Analysis of 487 patients revealed 16 oncogenic driver alterations, mostly amplifications, present in ≥5% of patients. Patients in the palliative-intent cohort, compared with those in the curative-intent cohort, were more likely to have metastatic disease, amplifications, Cell-cycle and RTK-RAS pathway alterations, as well as a higher fraction of genome altered and rate of whole-genome doubling. In multivariable analyses, alterations, alterations, amplifications, Cell-cycle and TGFβ pathways, and overall number of oncogenic drivers were independently associated with worse overall survival. amplification was associated with improved survival, presumably due to trastuzumab therapy.
Our study suggests that higher levels of genomic instability are associated with more advanced disease in esophageal adenocarcinoma. Furthermore, , and represent prognostic biomarkers, given their strong association with poor survival.
描绘食管腺癌中复发性致癌驱动因素改变和失调途径,并评估其预后价值。
我们分析了一组由 MSK-IMPACT 前瞻性测序的具有高质量临床注释的下段食管和食管胃交界腺癌患者的大型队列。根据治疗意图(根治性与姑息性)将患者细分,这与临床分期密切相关。使用 Cox 比例风险模型,根据诊断时可获得的相关临床病理因素,对全因生存进行调整,以评估基因组特征、改变和途径与全因生存的关联。
对 487 例患者的分析显示,16 种致癌驱动因素改变(主要为扩增)在≥5%的患者中存在。与根治性意向队列相比,姑息性意向队列的患者更有可能患有转移性疾病、扩增、细胞周期和 RTK-RAS 途径改变,以及更高比例的基因组改变和全基因组倍增率。在多变量分析中,改变、改变、扩增、细胞周期和 TGFβ途径以及致癌驱动因素的总数与较差的总生存独立相关。扩增与生存改善相关,可能归因于曲妥珠单抗治疗。
我们的研究表明,食管腺癌中更高水平的基因组不稳定性与更晚期的疾病相关。此外,、和代表预后生物标志物,因为它们与不良生存密切相关。
