Cancer Genomics Group, Vall d'Hebron Institute of Oncology (VHIO), Barcelona, Spain.
Gastrointestinal and Endocrine Tumor Unit, Vall d'Hebron Institute of Oncology (VHIO), Hospital Universitari Vall d'Hebron, Vall d'Hebron Barcelona Hospital Campus, Barcelona, Spain.
Clin Cancer Res. 2024 Oct 1;30(19):4491-4504. doi: 10.1158/1078-0432.CCR-23-3780.
FGFR2 fusions occur in 10% to 15% of patients with intrahepatic cholangiocarcinoma (iCCA), potentially benefiting from FGFR inhibitors (FGFRi). We aimed to assess the feasibility of detecting FGFR2 fusions in plasma and explore plasma biomarkers for managing FGFRi treatment.
We conducted a retrospective study in 18 patients with iCCA and known FGFR2 fusions previously identified in tissue samples from prior FGFRi treatment. Both tissue and synchronous plasma samples were analyzed using a custom hybrid capture gene panel with next-generation sequencing (VHIO-iCCA panel) and validated against commercial vendor results. Longitudinal plasma analysis during FGFRi was performed. Subsequently, we explored the correlation between plasma biomarkers, liver enzymes, tumor volume, and clinical outcomes.
Sixteen patients (88.9%) were positive for FGFR2 fusion events in plasma. Remarkably, the analysis of plasma suggests that lower levels of ctDNA are linked to clinical benefits from targeted therapy and result in improved progression-free survival and overall survival. Higher concentrations of cell-free DNA before FGFRi treatment were linked to worse overall survival, correlating with impaired liver function and indicating compromised cell-free DNA removal by the liver. Additionally, increased ctDNA or the emergence of resistance mutations allowed earlier detection of disease progression compared with standard radiologic imaging methods.
VHIO-iCCA demonstrated accurate detection of FGFR2 fusions in plasma. The integration of information from various plasma biomarkers holds the potential to predict clinical outcomes and identify treatment failure prior to radiologic progression, offering valuable guidance for the clinical management of patients with iCCA.
FGFR2 融合发生在 10%至 15%的肝内胆管癌(iCCA)患者中,可能受益于 FGFR 抑制剂(FGFRi)。我们旨在评估在血浆中检测 FGFR2 融合的可行性,并探索用于管理 FGFRi 治疗的血浆生物标志物。
我们对 18 名先前在 FGFRi 治疗前组织样本中已知 FGFR2 融合的 iCCA 患者进行了回顾性研究。使用定制的混合捕获基因panel 与下一代测序(VHIO-iCCA 面板)对组织和同步血浆样本进行分析,并与商业供应商的结果进行验证。在 FGFRi 期间进行了纵向血浆分析。随后,我们探讨了血浆生物标志物与肝酶、肿瘤体积和临床结果之间的相关性。
16 名患者(88.9%)的血浆中存在 FGFR2 融合事件。值得注意的是,血浆分析表明,较低水平的 ctDNA 与靶向治疗的临床获益相关,并导致无进展生存期和总生存期的改善。在 FGFRi 治疗前更高的游离 DNA 浓度与总生存期较差相关,与肝功能受损相关,并表明肝脏对游离 DNA 的清除受损。此外,ctDNA 的增加或耐药突变的出现可与标准放射成像方法相比更早地检测疾病进展。
VHIO-iCCA 成功检测到血浆中的 FGFR2 融合。整合来自各种血浆生物标志物的信息有可能预测临床结果,并在放射学进展之前识别治疗失败,为 iCCA 患者的临床管理提供有价值的指导。
