SCI
7 July 2024
Circulating Tumor DNA-Guided De-Escalation Targeted Therapy for Advanced Non−Small Cell Lung Cancer: A Nonrandomized Clinical Trial
(JAMA Oncology, IF: 22.5)
Song Dong, PhD; ZhenWang, PhD; Jia-Tao Zhang, PhD; Bingfa Yan, PhD; Chao Zhang, PhD; Xuan Gao, PhD; Hao Sun, PhD; Yang-Si Li, PhD; Hong-Hong Yan, MSc; Hai-Yan Tu, PhD; Si-Yang Maggie Liu, PhD; Yuhua Gong, PhD; Wei Gao, PhD; Jie Huang, PhD; Ri-Qiang Liao, PhD; Jun-Tao Lin, MD; E-E. Ke, PhD; Zelong Xu, PhD; Xue Zhang, PhD; Xuefeng Xia, PhD; An-Na Li, PhD; Si-Yang Liu, PhD; Yi Pan, PhD; Jin-Ji Yang, PhD; Wen-Zhao Zhong, PhD; Xin Yi, PhD; Qing Zhou, PhD; Xue-Ning Yang, PhD; Yi-LongWu, MD
CORRESPONDENCE TO: syylwu@live.cn, and yangxuening@gdph.org.cn
Uninterrupted targeted therapy until disease progression or intolerable toxic effects is currently the routine therapy for advanced non−small cell lung cancer (NSCLC) involving driver gene variations. However, drug resistance is inevitable.
不间断靶向治疗直到疾病进展或产生不可忍受的毒性作用是目前涉及驱动基因变异的晚期非小细胞肺癌(NSCLC)的常规治疗。然而,耐药性是不可避免的。
To assess the clinical feasibility of adaptive de-escalation tyrosine kinase inhibitor (TKI) treatment guided by circulating tumor DNA (ctDNA) for achieving complete remission after local consolidative therapy (LCT) in patients with advanced NSCLC.
评估以循环肿瘤DNA(ctDNA)为指导的适应性酪氨酸激酶抑制剂(TKI)治疗晚期非小细胞肺癌患者局部巩固治疗(LCT)后完全缓解的临床可行性。
This prospective nonrandomized trial was conducted at a single center from June 3, 2020, to July 19, 2022, and included 60 patients with advanced NSCLC with driver variations without radiologically detectable disease after TKI and LCT. The median (range) follow-up time was 19.2 (3.8-29.7) months. Data analysis was conducted from December 15, 2022, to May 10, 2023.
这项前瞻性非随机试验于2020年6月3日至2022年7月19日在一个中心进行,纳入了60名晚期非小细胞肺癌患者,这些患者在TKI和LCT治疗后没有放射学可检测到的疾病。中位(范围)随访时间为19.2(3.8-29.7)个月。数据分析于2022年12月15日至2023年5月10日进行。
Cessation of TKI treatment and follow-up every 3 months. Treatment was restarted in patients with progressive disease (defined by the Response Evaluation Criteria in Solid Tumors 1.1 criteria), detectable ctDNA, or elevated carcinoembryonic antigen (CEA) levels, whichever manifested first, and treatment ceased if all indicators were negative during follow-up surveillance.
停止TKI治疗后每3个月随访一次。对进展性疾病(由实体瘤反应评估标准1.1标准定义)、可检测的ctDNA或癌胚抗原(CEA)水平升高的患者重新开始治疗,以二者中先出现者为准,如果随访期间所有指标均为阴性,则停止治疗。
Progression-free survival (PFS). Secondary end points were objective response rate, time to next treatment, and overall survival.
无进展生存期(PFS)。次要终点是客观有效率、下次治疗时间和总生存率。
Among the total study sample of 60 participants (median [range] age, 55 [21-75] years; 33 [55%] were female), the median PFS was 18.4 (95%CI, 12.6-24.2) months and the median (range) total treatment break duration was 9.1 (1.5-28.1) months. Fourteen patients (group A) remained in TKI cessation with a median (range) treatment break duration of 20.3 (6.8-28.1) months; 31 patients (group B) received retreatment owing to detectable ctDNA and/or CEA and had a median PFS of 20.2 (95%CI, 12.9-27.4) months with a median (range) total treatment break duration of 8.8 (1.5-20.6) months; and 15 patients (group C) who underwent retreatment with TKIs due to progressive disease had a median PFS of 5.5 (95% CI, 1.5-7.2) months. For all participants, the TKI retreatment response rate was 96%, the median time to next treatment was 29.3 (95%CI, 25.3-35.2) months, and the data for overall survival were immature.
在60名参与者的总研究样本中(中位[范围]年龄,55[21-75]岁;33人[55%]为女性),中位PFS为18.4(95%CI,12.6-24.2)个月,中位(范围)总治疗中断时间为9.1(1.5-28.1)个月。14名患者(A组)仍处于TKI停止期,中位(范围)治疗中断时间为20.3(6.8-28.1)个月;31名患者(B组)因可检测的ctDNA和/或CEA水平而接受了再治疗,中位PFS为20.2(95%CI,12.9-27.4)个月,中位(范围)总治疗中断时间为8.8(1.5-20.6)个月;15名因疾病进展而接受TKIs再治疗的患者(C组)的中位PFS为5.5(95%CI,1.5-7.2)个月。对于所有参与者,TKI再治疗有效率为96%,下一次治疗的中位时间为29.3个月(95%CI,25.3-35.2),总体生存率数据尚不成熟。
The findings of this nonrandomized trial suggest that this adaptive de-escalation TKI strategy for patients with NSCLC is feasible in those with no lesions after LCT and a negative ctDNA test result. This might provide a de-escalation treatment strategy guided by ctDNA for the subset of patients with advanced NSCLC.
这项非随机试验的结果表明,这种针对NSCLC患者的适应性降级TKI策略在LCT后无病变且ctDNA检测结果呈阴性的患者中是可行的。这可能为晚期NSCLC患者提供一种以ctDNA为指导的降级治疗策略。
