Department of Medicine I, Clinical Division of Oncology, Medical University of Vienna, Spitalgasse 23, 1090, Vienna, Austria.
Comprehensive Cancer Center Vienna, Vienna, Austria.
Hepatol Int. 2020 Mar;14(2):288-295. doi: 10.1007/s12072-020-10020-6. Epub 2020 Feb 25.
Advanced therapy-refractory biliary tract cancer (BTC) has poor prognosis and constitutes a major challenge for adequate treatment strategies. By mapping the molecular profiles of advanced BTC patients, precision cancer medicine may provide targeted therapies for these patients.
In this analysis, we aimed to show the potential of PCM in metastatic BTC.
In this single-center, real-world retrospective analysis of our PCM platform, we describe the molecular profiling of 30 patients diagnosed with different types of metastatic BTC. Tumor samples of the patients were examined using a 161-gene next-generation sequencing panel, immunohistochemistry (IHC), and fluorescence in situ hybridization for chromosomal translocations.
In total, we identified 35 molecular aberrations in 30 patients. The predominant mutations were KRAS (n = 8), TP53 (n = 7), IDH2 (n = 4), and IDH1 (n = 3) that accounted for the majority of all molecular alterations (62.86%). BRAF mutations were observed in two patients. Less frequent alterations were noted in ARID1A, CTNNB1, ESR1, FBXW7, FGFR2, MET, NOTCH2, PIK3CA, PTCH1, SMAD4, and SRC1, each in one case. FGFR fusion gene was detected in one patient. No mutations were detected in eight patients. IHC revealed EGFR and p-mTOR expression in 28 patients. Applying these results to our patients, targeted therapy was recommended for 60% of the patients (n = 18). One patient achieved stable disease.
PCM is a feasible treatment approach and may provide molecular-guided therapy recommendations for metastatic BTC.
晚期治疗难治性胆道癌(BTC)预后差,是充分治疗策略的主要挑战。通过对晚期 BTC 患者的分子谱进行绘图,精准癌症医学可能为这些患者提供靶向治疗。
在这项分析中,我们旨在展示精准癌症医学在转移性 BTC 中的潜力。
在我们的精准癌症医学平台的这项单中心、真实世界回顾性分析中,我们描述了 30 名不同类型转移性 BTC 患者的分子分析情况。使用 161 基因下一代测序面板、免疫组织化学(IHC)和染色体易位荧光原位杂交对患者的肿瘤样本进行了检查。
我们共在 30 名患者中鉴定出 35 种分子异常。主要突变是 KRAS(n=8)、TP53(n=7)、IDH2(n=4)和 IDH1(n=3),这些突变占所有分子改变的大部分(62.86%)。两名患者观察到 BRAF 突变。ARID1A、CTNNB1、ESR1、FBXW7、FGFR2、MET、NOTCH2、PIK3CA、PTCH1、SMAD4 和 SRC1 也分别在一名患者中出现较少见的改变。一名患者检测到 FGFR 融合基因。8 名患者未检测到突变。IHC 显示 28 名患者存在 EGFR 和 p-mTOR 表达。根据这些结果向我们的患者推荐靶向治疗,推荐 60%的患者(n=18)接受靶向治疗。一名患者病情稳定。
精准癌症医学是一种可行的治疗方法,可为转移性 BTC 提供基于分子的治疗建议。