免疫疗法在致癌基因驱动的非小细胞肺癌患者中的疗效:一项系统评价和荟萃分析。
Efficacy of immunotherapy in patients with oncogene-driven non-small-cell lung cancer: a systematic review and meta-analysis.
作者信息
Chen Jiayan, Lu Wanjun, Chen Mo, Cai Zijing, Zhan Ping, Liu Xin, Zhu Suhua, Ye Mingxiang, Lv Tangfeng, Lv Jiawen, Song Yong, Wang Dong
机构信息
Department of Respiratory and Critical Care Medicine, Jinling Hospital, Nanjing Medical University, Nanjing, Jiangsu, China.
Department of Respiratory and Critical Care Medicine, Jinling Hospital, Medical School of Nanjing University, Nanjing, Jiangsu, China.
出版信息
Ther Adv Med Oncol. 2024 Feb 27;16:17588359231225036. doi: 10.1177/17588359231225036. eCollection 2024.
BACKGROUND
Immunotherapy is an emerging antitumor therapy that can improve the survival of patients with advanced non-small-cell lung cancer (NSCLC). However, only about 20% of NSCLC patients can benefit from this treatment. At present, whether patients with driving gene-positive NSCLC can benefit from immunotherapy is one of the hot issues. Therefore, we conducted a meta-analysis to evaluate the efficacy of immunotherapy in patients with oncogene-driven NSCLC and concluded the efficacy of altered subtypes.
METHODS
A literature search was performed using PubMed, Web of Science, and Cochrane databases. The primary endpoints included the objective response rate (ORR), median progression-free survival (mPFS), and median overall survival (mOS) in patients with oncogene-driven NSCLC.
RESULTS
In all, 86 studies involving 4524 patients with oncogene-driven NSCLC were included in this meta-analysis. The pooled ORRs in clinical trials treated with monoimmunotherapy of EGFR, ALK, and KRAS alteration were 6%, 0%, and 23%, respectively. In retrospective studies, the pooled ORRs of EGFR, ALK, KRAS, BRAF, MET, HER2, RET, and ROS1 alteration were 8%, 3%, 28%, 24%, 23%, 14%, 7%, and 8%, respectively. Among them, the pooled ORRs of KRAS non-G12C mutation, KRAS G12C mutation, BRAF V600E mutation, BRAF non-V600E mutation, MET-exon 14 skipping, and MET-amplification were 33% 40%, 20%, 34%, 17%, and 60%, respectively. In addition, the pooled mPFS rates of EGFR, KRAS, MET, HER2, and RET alteration were 2.77, 3.24, 2.48, 2.31, and 2.68 months, while the pooled mOS rates of EGFR and KRAS alteration were 9.98 and 12.29 months, respectively. In prospective data concerning EGFR mutation, the pooled ORR and mPFS treated with chemo-immunotherapy (IC) reached 38% and 6.20 months, while 58% and 8.48 months with chemo-immunotherapy plus anti-angiogenesis therapy (ICA). Moreover, the pooled mPFS and mOS of monoimmunotherapy was 2.33 months and 12.43 months.
CONCLUSIONS
, and -altered NSCLC patients have poor reactivity to monoimmunotherapy but the efficacy of immune-based combined therapy is significantly improved. G12C mutation, non-V600E mutation, and amplification have better responses to immunotherapy, and more prospective studies are needed for further research.
背景
免疫疗法是一种新兴的抗肿瘤疗法,可提高晚期非小细胞肺癌(NSCLC)患者的生存率。然而,只有约20%的NSCLC患者能从这种治疗中获益。目前,驱动基因阳性的NSCLC患者是否能从免疫疗法中获益是热点问题之一。因此,我们进行了一项荟萃分析,以评估免疫疗法在致癌基因驱动的NSCLC患者中的疗效,并总结不同亚型改变的疗效。
方法
使用PubMed、Web of Science和Cochrane数据库进行文献检索。主要终点包括致癌基因驱动的NSCLC患者的客观缓解率(ORR)、中位无进展生存期(mPFS)和中位总生存期(mOS)。
结果
本荟萃分析共纳入86项研究,涉及4524例致癌基因驱动的NSCLC患者。在接受EGFR、ALK和KRAS改变的单免疫疗法治疗的临床试验中,汇总的ORR分别为6%、0%和23%。在回顾性研究中,EGFR、ALK、KRAS、BRAF、MET、HER2、RET和ROS1改变的汇总ORR分别为8%、3%、28%、24%、23%、14%、7%和8%。其中,KRAS非G12C突变、KRAS G12C突变、BRAF V600E突变、BRAF非V600E突变、MET外显子14跳跃和MET扩增的汇总ORR分别为33%、40%、20%、34%、17%和60%。此外,EGFR、KRAS、MET、HER2和RET改变的汇总mPFS率分别为2.77、3.24、2.48、2.31和2.68个月,而EGFR和KRAS改变的汇总mOS率分别为9.98和12.29个月。在关于EGFR突变的前瞻性数据中,化疗免疫疗法(IC)治疗的汇总ORR和mPFS分别达到38%和6.20个月,而化疗免疫疗法联合抗血管生成疗法(ICA)则为58%和8.48个月。此外,单免疫疗法的汇总mPFS和mOS分别为2.33个月和12.43个月。
结论
EGFR、ALK和ROS1改变的NSCLC患者对单免疫疗法反应较差,但基于免疫的联合疗法疗效显著提高。KRAS G12C突变、BRAF非V600E突变和MET扩增对免疫疗法反应较好,需要更多前瞻性研究进行进一步探究。
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