Tudor Roxana Alina, D'Silva Adrijana, Tremblay Alain, MacEachern Paul, Morris Don, Brenner Darren, Kopciuk Karen, Bebb Dafydd Gwyn
Department of Medical Oncology, Cumming School of Medicine, University of Calgary, Calgary-Alberta, Canada.
Division of Respiratory Medicine, Cumming School of Medicine, University of Calgary, Calgary-Alberta, Canada.
PLoS One. 2017 Aug 4;12(8):e0181867. doi: 10.1371/journal.pone.0181867. eCollection 2017.
Treatment and clinical-outcomes were described in a sub-cohort of non-small-cell lung cancer (NSCLC) patients with disease-progression (PD) after epidermal growth factor tyrosine kinase inhibitors (EGFR-TKIs) treatment.
We retrospectively analyzed a single-institutional EGFR mutation positive (EGFRmut+) NSCLC cohort for post-TKI-PD management, and assessed overall survival (OS) and post-progression survival (PPS). All de-novo (first lung-cancer occurrence) stage IIIA-IV patients, as well as de-novo stage IV subset was analyzed. Multi-state modeling (MSM) and a Cox PH regression model with propensity score weights adjusted for clinicopathological variables between: diagnosis and PD and PD to death.
123 stage IIIA-IV patients were identified with 104 meeting RECIST-1.1-PD criteria. This RECIST-1.1-PD criteria subset included females (64.6%), Asians (39.4%), never/non-smokers (55.8%), and exon 19 deletion carriers (44.2%). Commonest treatment beyond initial-PD was continuing TKI alone (46/104), with another 21 patients continuing TKI plus additional systemic therapy. The median OS for patients who continued TKI treatment at initial-PD was 21.1 months versus 15.6 months for patients who discontinued TKI, p = 0.006. Via MSM analysis, continuing TKI at initial-PD followed by other systemic therapy was associated with an 83% reduced death risk, adjusted HR: 0.17 (95% CI: 0.07, 0.39). In the Cox PH model, ever-smokers with an exon 19 deletion had increased risk of death after PD (adjusted HR: 3.19, 95% CI: 1.54, 6.58), as did exon 21 mutation carriers, (adjusted HR: 2.10, 95% CI: 1.10, 4.00) and females (adjusted HR: 3.19, 95% CI: 1.54, 6.58).
Subsequent systemic therapy after continuing TKI at initial-PD reduced the risk of death. Additionally, our data suggest that positive smoking history increases death risk for some EGFR mutation types and females.
描述一组非小细胞肺癌(NSCLC)患者在接受表皮生长因子酪氨酸激酶抑制剂(EGFR-TKIs)治疗后疾病进展(PD)的治疗情况及临床结局。
我们回顾性分析了一个单机构的EGFR突变阳性(EGFRmut+)NSCLC队列,以进行TKI治疗后疾病进展的管理,并评估总生存期(OS)和疾病进展后生存期(PPS)。分析了所有初发(首次发生肺癌)的IIIA-IV期患者以及初发IV期亚组。采用多状态建模(MSM)和Cox PH回归模型,对诊断至疾病进展以及疾病进展至死亡之间的临床病理变量进行倾向评分加权调整。
共确定了123例IIIA-IV期患者,其中104例符合RECIST-1.1-PD标准。该RECIST-1.1-PD标准亚组包括女性(64.6%)、亚洲人(39.4%)、从不吸烟者/非吸烟者(55.8%)以及外显子19缺失携带者(44.2%)。初始疾病进展后最常见的治疗方法是单独继续使用TKI(46/104),另有21例患者继续使用TKI并联合其他全身治疗。初始疾病进展时继续使用TKI治疗的患者中位总生存期为21.1个月,而停用TKI的患者为15.6个月,p = 0.006。通过MSM分析,初始疾病进展时继续使用TKI然后接受其他全身治疗与死亡风险降低83%相关,调整后风险比(HR):0.17(95%置信区间:0.07,0.39)。在Cox PH模型中,外显子19缺失的曾经吸烟者在疾病进展后的死亡风险增加(调整后HR:3.19,95%置信区间:1.54,6.58),外显子21突变携带者也是如此(调整后HR:2.10,95%置信区间:1.10,4.00),女性也是如此(调整后HR:3.19,95%置信区间:1.54,6.58)。
初始疾病进展时继续使用TKI后进行后续全身治疗可降低死亡风险。此外,我们的数据表明,阳性吸烟史会增加某些EGFR突变类型和女性的死亡风险。
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