Wu Jia-Jun, Zheng Zhe-Rong, Lo Tse-Hsien, Chu Cheng-Hsiang, Chen Kun-Chieh, Chang Gee-Chen
Institute of Medicine, Chung Shan Medical University, Taichung, Taiwan.
School of Medicine, Chung Shan Medical University, Taichung, Taiwan.
JTO Clin Res Rep. 2025 Apr 9;6(6):100832. doi: 10.1016/j.jtocrr.2025.100832. eCollection 2025 Jun.
Dysregulated signaling, such as MET overexpression or amplification (amp), is a important mechanism of resistance to EGFR tyrosine kinase inhibitors (TKIs) in patients with -mutant lung adenocarcinoma (LUAD). Combination therapy with EGFR TKIs and MET TKIs has revealed efficacy in these patients. This study aimed to analyze the real-world experience of TKI combination in patients with -mutant MET-overexpressed LUAD.
This retrospective cohort study included patients with advanced -mutant LUAD who progressed after EGFR TKIs and were treated with combination therapy of EGFR TKIs and MET TKIs (capmatinib or tepotinib). Immunohistochemistry was used to detect MET overexpression.
This study included 27 patients, with a median age of 69 years; 40.7% of the patients were male individuals, and 88.9% never smoked. Overall, the treatment response of the TKI combination reported 29.6% (eight of 27) partial response, 55.6% (15 of 27) stable disease, a median progression-free survival of 7.3 months, and an overall survival of 26.9 months. The adverse events were mostly grade 1 to 2, with only one patient experiencing a grade 3 or greater event, which was peripheral edema. The most common adverse events were hypoalbuminemia (44.4%), increased creatinine (44.4%), and peripheral edema (44.4%). Eight patients underwent next-generation sequencing analysis, and two (25.0%) of them had amp. Three patients (37.5%) had mutations, which were the most common concurrent alterations. Those with positive amp had significantly longer median progression-free survival than those without (25.3 versus 5.8 mo; = 0.034).
The TKI combination reported clinical activities in patients with advanced -mutant LUAD resistant to EGFR TKIs and mild toxicity in those with MET overexpression.
信号失调,如MET过表达或扩增,是EGFR酪氨酸激酶抑制剂(TKI)治疗伴有EGFR突变的肺腺癌(LUAD)患者耐药的重要机制。EGFR TKI与MET TKI联合治疗已显示出对这些患者有效。本研究旨在分析TKI联合治疗伴有EGFR突变且MET过表达的LUAD患者的真实世界经验。
这项回顾性队列研究纳入了晚期EGFR突变的LUAD患者,这些患者在接受EGFR TKI治疗后病情进展,并接受了EGFR TKI与MET TKI(卡马替尼或替泊替尼)联合治疗。采用免疫组织化学检测MET过表达。
本研究纳入27例患者,中位年龄69岁;40.7%为男性,88.9%从不吸烟。总体而言,TKI联合治疗的反应报告显示,部分缓解率为29.6%(27例中的8例),疾病稳定率为55.6%(27例中的15例),无进展生存期的中位数为7.3个月,总生存期为26.9个月。不良事件大多为1至2级,只有1例患者发生3级或更高级别的事件,即外周水肿。最常见的不良事件为低白蛋白血症(44.4%)、肌酐升高(44.4%)和外周水肿(44.4%)。8例患者接受了二代测序分析,其中2例(25.0%)有扩增。3例患者(37.5%)有其他突变,这是最常见的并发改变。有扩增阳性的患者无进展生存期的中位数显著长于无扩增的患者(25.3个月对5.8个月;P = 0.034)。
TKI联合治疗对晚期EGFR突变且对EGFR TKI耐药的LUAD患者显示出临床活性,对MET过表达的患者毒性较轻。
