EGFR 突变型非小细胞肺癌患者(序贯)再活检中 T790M 突变的发生率。
Incidence of T790M mutation in (sequential) rebiopsies in EGFR-mutated NSCLC-patients.
机构信息
Department of Pulmonary Diseases, VU University Medical Center, Amsterdam, The Netherlands.
Department of Pathology, VU University Medical Center, Amsterdam, The Netherlands.
出版信息
Lung Cancer. 2014 Jul;85(1):19-24. doi: 10.1016/j.lungcan.2014.03.016. Epub 2014 Mar 23.
AIM
Non-small cell lung cancer (NSCLC)-patients with an epidermal growth factor receptor (EGFR)-mutation have median progression-free survival (PFS) of 12 months on tyrosine kinase inhibitors (TKIs). Resistance is mediated by the EGFR T790M-mutation in the majority of patients. Longitudinal follow-up data are lacking. We retrospectively evaluated EGFR-mutated NSCLC-patients who were rebiopsied after TKI-treatment. A subgroup was sequentially rebiopsied along the course of the disease.
PATIENTS AND METHODS
Advanced EGFR-mutated NSCLC-patients who had both a pre-TKI biopsy and post-TKI biopsy available were included. Information on treatments and (re)biopsies was collected chronologically. Primary endpoint was the incidence of the T790M-mutation.
RESULTS
Sixty-six patients fulfilled the inclusion criteria. In first post-TKI biopsies, T790M-mutation was detected in 34 patients (52%) of patients. Twenty-seven patients had subsequent post-TKI rebiopsies with mutation analysis available; in 10 patients (37%) the T790M-status in subsequent post-TKI rebiopsies was not consistent with the T790M-status of the first post-TKI biopsy. Progression free survival (PFS) on TKI-treatment was 12.0 months. Objective response rate on TKI-treatment was 81%. Patients developing T790M-mutation at post-TKI biopsy had longer median PFS compared to T790M-negative patients (14.2 versus 11.1 months respectively (P=0.034)) and longer overall survival (45.9 months versus 29.8 months respectively (P=0.213)). Transformation to SCLC was detected in 1 patient (2%).
CONCLUSION
Incidence of T790M-mutation at first post-TKI biopsy in this cohort of EGFR-mutated NSCLC-patients was 52%. Detection of T790M-mutation was not consistent over time; some patients who were T790M-positive at first post-TKI biopsy became T790M-negative in later post-TKI rebiopsies and vice versa. T790M-positive patients showed longer PFS than T790M-negative patients. Whether the low incidence of transformation to SCLC is justifying post-TKI rebiopsy in EGFR-mutated NSCLC-patients with acquired TKI-resistance in regular clinical practice is debatable.
目的
表皮生长因子受体(EGFR)突变的非小细胞肺癌(NSCLC)患者在酪氨酸激酶抑制剂(TKI)治疗下的无进展生存期(PFS)中位数为 12 个月。大多数患者的耐药性是由 EGFR T790M 突变介导的。目前缺乏纵向随访数据。我们回顾性评估了 EGFR 突变型 NSCLC 患者,这些患者在 TKI 治疗后进行了再活检。其中一个亚组在疾病过程中进行了连续再活检。
患者和方法
纳入了既有 TKI 治疗前活检又有 TKI 治疗后活检的晚期 EGFR 突变型 NSCLC 患者。按时间顺序收集有关治疗和(再)活检的信息。主要终点是 T790M 突变的发生率。
结果
66 名患者符合纳入标准。在首次 TKI 治疗后的活检中,34 名患者(52%)检测到 T790M 突变。27 名患者随后进行了 TKI 治疗后有基因突变分析的再次活检;在 10 名患者(37%)中,T790M 状态在随后的 TKI 治疗后再次活检中与 TKI 治疗后的首次活检不一致。TKI 治疗的无进展生存期(PFS)为 12.0 个月。TKI 治疗的客观缓解率为 81%。与 T790M 阴性患者相比,在 TKI 治疗后活检中出现 T790M 突变的患者的中位 PFS 更长(分别为 14.2 个月和 11.1 个月(P=0.034)),总生存期更长(分别为 45.9 个月和 29.8 个月(P=0.213))。在 1 名患者(2%)中检测到小细胞肺癌转化。
结论
在这组 EGFR 突变型 NSCLC 患者中,首次 TKI 治疗后活检中 T790M 突变的发生率为 52%。随着时间的推移,T790M 突变的检测结果并不一致;一些在首次 TKI 治疗后活检中 T790M 阳性的患者在随后的 TKI 治疗后再次活检中变成了 T790M 阴性,反之亦然。T790M 阳性患者的 PFS 长于 T790M 阴性患者。在常规临床实践中,对于获得性 TKI 耐药的 EGFR 突变型 NSCLC 患者,低发生率的转化为小细胞肺癌是否证明 TKI 治疗后再次活检是合理的,这是有争议的。
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