同步放化疗治疗局部晚期非小细胞肺癌患者采用免疫治疗巩固前后的肺炎发生率
Pneumonitis Rates Before and After Adoption of Immunotherapy Consolidation in Patients With Locally Advanced Non-Small Cell Lung Cancer Treated With Concurrent Chemoradiation.
作者信息
Yegya-Raman Nikhil, Friedes Cole, Lee Sang Ho, Iocolano Michelle, Duan Lian, Wang Xingmei, Li Bolin, Aggarwal Charu, Cohen Roger B, Su William, Doucette Abigail, Levin William P, Cengel Keith A, DiBardino David, Teo Boon-Keng Kevin, O'Reilly Shannon E, Sun Lova, Bradley Jeffrey D, Xiao Ying, Langer Corey J, Feigenberg Steven J
机构信息
Departments of Radiation Oncology.
Departments of Radiation Oncology.
出版信息
Int J Radiat Oncol Biol Phys. 2024 Apr 1;118(5):1445-1454. doi: 10.1016/j.ijrobp.2023.08.039. Epub 2023 Aug 22.
PURPOSE
We hypothesized that after adoption of immune checkpoint inhibitor (ICI) consolidation for patients with locally advanced non-small cell lung cancer (LA-NSCLC) receiving concurrent chemoradiation therapy (cCRT), rates of symptomatic pneumonitis would increase, thereby supporting efforts to reduce lung radiation dose.
METHODS AND MATERIALS
This single institution, multisite retrospective study included 783 patients with LA-NSCLC treated with definitive cCRT either before introduction of ICI consolidation (pre-ICI era cohort [January 2011-September 2017]; N = 448) or afterward (ICI era cohort [October 2017-December 2021]; N = 335). Primary endpoint was grade ≥2 pneumonitis (G2P) and secondary endpoint was grade ≥3 pneumonitis (G3P), per Common Terminology Criteria for Adverse Events v5.0. Pneumonitis was compared between pre-ICI era and ICI era cohorts using the cumulative incidence function and Gray's test. Inverse probability of treatment weighting (IPTW)-adjusted Fine-Gray models were generated. Logistic models were developed to predict the 1-year probability of G2P as a function of lung dosimetry.
RESULTS
G2P was higher in the ICI era than in the pre-ICI era (1-year cumulative incidence 31.4% vs 20.1%; P < .001; IPTW-adjusted multivariable subdistribution hazard ratio, 2.03; 95% confidence interval, 1.53-2.70; P < .001). There was no significant interaction between ICI era treatment and either lung volume receiving ≥20 Gy (V20) or mean lung dose in Fine-Gray regression for G2P; however, the predicted probability of G2P was higher in the ICI era at clinically relevant values of lung V20 (≥24%) and mean lung dose (≥14 Gy). Cut-point analysis revealed a lung V20 threshold of 28% in the ICI era (1-year G2P rate 46.0% above vs 19.8% below; P < .001). Among patients receiving ICI consolidation, lung V5 was not associated with G2P. G3P was not higher in the ICI era (1-year cumulative incidence 7.5% vs 6.0%; P = .39; IPTW-adjusted multivariable subdistribution hazard ratio, 1.12; 95% confidence interval, 0.63-2.01; P = .70).
CONCLUSIONS
In patients with LA-NSCLC treated with cCRT, the adoption of ICI consolidation was associated with an increase in G2P but not G3P. With ICI consolidation, stricter lung dose constraints may be warranted.
目的
我们假设,对于接受同步放化疗(cCRT)的局部晚期非小细胞肺癌(LA-NSCLC)患者,采用免疫检查点抑制剂(ICI)巩固治疗后,症状性肺炎的发生率会增加,从而支持降低肺部辐射剂量的努力。
方法和材料
这项单机构、多中心回顾性研究纳入了783例接受确定性cCRT治疗的LA-NSCLC患者,这些患者在引入ICI巩固治疗之前(ICI前时代队列[2011年1月至2017年9月];N = 448)或之后(ICI时代队列[2017年10月至2021年12月];N = 335)接受治疗。根据不良事件通用术语标准第5.0版,主要终点是≥2级肺炎(G2P),次要终点是≥3级肺炎(G3P)。使用累积发病率函数和Gray检验比较ICI前时代和ICI时代队列之间的肺炎情况。生成了逆概率加权(IPTW)调整后的Fine-Gray模型。开发了逻辑模型来预测G2P的1年概率作为肺剂量测定的函数。
结果
ICI时代的G2P高于ICI前时代(1年累积发病率31.4%对20.1%;P <.001;IPTW调整后的多变量亚分布风险比,2.03;95%置信区间,1.53 - 2.70;P <.001)。在G2P的Fine-Gray回归中,ICI时代治疗与接受≥20 Gy(V20)的肺体积或平均肺剂量之间没有显著相互作用;然而,在肺V20(≥24%)和平均肺剂量(≥14 Gy)的临床相关值时,ICI时代G2P的预测概率更高。切点分析显示,ICI时代肺V20阈值为28%(1年G2P率高于阈值时为46.0%,低于阈值时为19.8%;P <.001)。在接受ICI巩固治疗的患者中,肺V5与G2P无关。ICI时代的G3P没有更高(1年累积发病率7.5%对6.0%;P =.39;IPTW调整后的多变量亚分布风险比,1.12;95%置信区间,0.63 - 2.01;P =.70)。
结论
在接受cCRT治疗 的LA-NSCLC患者中,采用ICI巩固治疗与G2P增加相关,但与G3P无关。对于ICI巩固治疗,可能需要更严格的肺剂量限制。
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