Department of Medical Oncology, Dana-Farber Cancer Institute, Boston, Massachusetts.
Department of Medicine, Northwestern University, Chicago, Illinois.
Clin Cancer Res. 2023 Aug 15;29(16):2979-2987. doi: 10.1158/1078-0432.CCR-22-2189.
Acquired RET fusions have been reported at resistance to treatment with EGFR inhibitors in EGFR-mutant non-small cell lung cancer (NSCLC); however, a multicenter cohort of patients with EGFR-mutant lung cancers treated with osimertinib and selpercatinib for RET fusion-mediated osimertinib resistance has not previously been published.
Patients who received selpercatinib in combination with osimertinib on a prospective expanded access clinical trial (NCT03906331) and single-patient compassionate use programs across five countries were centrally analyzed. All patients had advanced EGFR-mutant NSCLC with a RET fusion detected from tissue or plasma following osimertinib therapy. Clinicopathologic and outcomes data were collected.
Fourteen patients with EGFR-mutant and RET fusion-positive lung cancers who experienced prior progression on osimertinib received osimertinib and selpercatinib. EGFR exon 19 deletions (±T790M, 86%) and non-KIF5B fusions (CCDC6-RET 50%, NCOA4-RET 36%) predominated. Osimertinib 80 mg daily and selpercatinib 80 mg twice daily were the most commonly administered dosages. The response rate, disease control rate, and median treatment duration were 50% [95% confidence interval (CI), 25%-75%, n = 12], 83% (95% CI, 55%-95%), and 7.9 months (range, 0.8-25+), respectively. Resistance was complex, involving EGFR on-target (EGFR C797S), RET on-target (RET G810S), and off-target (EML4-ALK/STRN-ALK, KRAS G12S, BRAF V600E) mechanisms; RET fusion loss; or polyclonal mechanisms.
For patients with EGFR-mutant NSCLC with an acquired RET fusion as a mechanism of EGFR inhibitor resistance, the addition of selpercatinib to osimertinib was feasible and safe and offered clinical benefit, supporting the prospective evaluation of this combination. See related commentary by Krebs and Popat, p. 2951.
已报道获得性 RET 融合可导致 EGFR 突变型非小细胞肺癌(NSCLC)患者对 EGFR 抑制剂治疗产生耐药;然而,此前尚未发表过接受奥希替尼和塞普替尼治疗 RET 融合介导的奥希替尼耐药的 EGFR 突变型肺癌患者的多中心队列研究结果。
对一项前瞻性扩大准入临床试验(NCT03906331)和 5 个国家的单个患者同情使用计划中接受塞普替尼联合奥希替尼治疗的患者进行中心分析。所有患者均为晚期 EGFR 突变型 NSCLC,在奥希替尼治疗后从组织或血浆中检测到 RET 融合。收集临床病理和结局数据。
14 例先前接受奥希替尼治疗后进展的 EGFR 突变型和 RET 融合阳性肺癌患者接受了奥希替尼和塞普替尼治疗。EGFR 外显子 19 缺失(±T790M,86%)和非 KIF5B 融合(CCDC6-RET 50%,NCOA4-RET 36%)为主。最常使用的奥希替尼剂量为 80 mg 每日 1 次,塞普替尼剂量为 80 mg 每日 2 次。客观缓解率、疾病控制率和中位治疗持续时间分别为 50%(95%置信区间[CI],25%-75%,n=12)、83%(95%CI,55%-95%)和 7.9 个月(范围:0.8-25+)。耐药机制复杂,包括 EGFR 靶上(EGFR C797S)、RET 靶上(RET G810S)和非靶上(EML4-ALK/STRN-ALK、KRAS G12S、BRAF V600E)、RET 融合丢失或多克隆耐药机制。
对于获得性 RET 融合作为 EGFR 抑制剂耐药机制的 EGFR 突变型 NSCLC 患者,奥希替尼联合塞普替尼是可行和安全的,并提供了临床获益,支持对此类联合治疗进行前瞻性评估。详见 Krebs 和 Popat 的相关评论,第 2951 页。
