1 National Cancer Centre Singapore, Singapore.
2 Singapore General Hospital, Singapore.
J Clin Oncol. 2019 Apr 10;37(11):876-884. doi: 10.1200/JCO.18.00177. Epub 2019 Jan 24.
Mesenchymal epithelial transition factor ( MET) activation has been implicated as an oncogenic driver in epidermal growth factor receptor ( EGFR)-mutant non-small-cell lung cancer (NSCLC) and can mediate primary and secondary resistance to EGFR tyrosine kinase inhibitors (TKI). High copy number thresholds have been suggested to enrich for response to MET inhibitors. We examined the clinical relevance of MET copy number gain (CNG) in the setting of treatment-naive metastatic EGFR-mutant-positive NSCLC.
MET fluorescence in situ hybridization was performed in 200 consecutive patients identified as metastatic treatment-naïve EGFR-mutant-positive. We defined MET-high as CNG greater than or equal to 5, with an additional criterion of MET/centromeric portion of chromosome 7 ratiο greater than or equal to 2 for amplification. Time-to-treatment failure (TTF) to EGFR TKI in patients identified as MET-high and -low was estimated by Kaplan-Meier method and compared using log-rank test. Multiregion single-nucleotide polymorphism array analysis was performed on 13 early-stage resected EGFR-mutant-positive NSCLC across 59 sectors to investigate intratumoral heterogeneity of MET CNG.
Fifty-two (26%) of 200 patients in the metastatic cohort were MET-high at diagnosis; 46 (23%) had polysomy and six (3%) had amplification. Median TTF was 12.2 months (95% CI, 5.7 to 22.6 months) versus 13.1 months (95% CI, 10.6 to 15.0 months) for MET-high and -low, respectively ( P = .566), with no significant difference in response rate regardless of copy number thresholds. Loss of MET was observed in three of six patients identified as MET-high who underwent postprogression biopsies, which is consistent with marked intratumoral heterogeneity in MET CNG observed in early-stage tumors. Suboptimal response (TTF, 1.0 to 6.4 months) to EGFR TKI was observed in patients with coexisting MET amplification (five [3.2%] of 154).
Although up to 26% of TKI-naïve EGFR-mutant-positive NSCLC harbor high MET CNG by fluorescence in situ hybridization, this did not significantly affect response to TKI, except in patients identified as MET-amplified. Our data underscore the limitations of adopting arbitrary copy number thresholds and the need for cross-assay validation to define therapeutically tractable MET pathway dysregulation in EGFR-mutant-positive NSCLC.
间质上皮转化因子(MET)的激活被认为是表皮生长因子受体(EGFR)突变型非小细胞肺癌(NSCLC)中的致癌驱动因素,并且可以介导对 EGFR 酪氨酸激酶抑制剂(TKI)的原发性和继发性耐药。已经提出高拷贝数阈值可以富集对 MET 抑制剂的反应。我们在未经治疗的转移性 EGFR 突变阳性 NSCLC 的背景下研究了 MET 拷贝数增益(CNG)的临床相关性。
对 200 例经鉴定为转移性初治 EGFR 突变阳性的患者进行了 MET 荧光原位杂交。我们将 MET 高定义为 CNG 大于或等于 5,并且 MET/7 号染色体着丝粒部分的比值大于或等于 2 用于扩增。通过 Kaplan-Meier 法估计 MET-high 和 -low 患者的 EGFR TKI 治疗失败时间(TTF),并通过对数秩检验进行比较。对 59 个区的 13 例早期切除的 EGFR 突变阳性 NSCLC 进行了多区域单核苷酸多态性阵列分析,以研究 MET CNG 的肿瘤内异质性。
在转移性队列的 200 例患者中,52 例(26%)在诊断时为 MET-high;46 例(23%)为多倍体,6 例(3%)为扩增。MET-high 和 -low 的中位 TTF 分别为 12.2 个月(95%CI,5.7 至 22.6 个月)和 13.1 个月(95%CI,10.6 至 15.0 个月)(P=.566),无论拷贝数阈值如何,反应率均无显著差异。在 6 例经证实为 MET-high 的患者中,有 3 例在接受进展后活检时观察到 MET 丢失,这与早期肿瘤中观察到的 MET CNG 明显的肿瘤内异质性一致。在共存 MET 扩增的患者中(154 例中的 5 例[3.2%]),观察到对 EGFR TKI 的次优反应(TTF,1.0 至 6.4 个月)。
尽管通过荧光原位杂交,多达 26%的初治 EGFR 突变阳性 NSCLC 存在高 MET CNG,但这并未显著影响 TKI 的反应,除了在经证实为 MET 扩增的患者中。我们的数据强调了采用任意拷贝数阈值的局限性,以及需要进行交叉检测验证来确定 EGFR 突变阳性 NSCLC 中治疗可行的 MET 途径失调。
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