基于血液的蛋白质组分析在晚期非小细胞肺癌一线免疫治疗中的真实世界疗效。
Real-world performance of blood-based proteomic profiling in first-line immunotherapy treatment in advanced stage non-small cell lung cancer.
机构信息
Lung Cancer, Piedmont Physicians Group, Atlanta, Georgia, USA.
Virginia Cancer Institute, Richmond, Virginia, USA.
出版信息
J Immunother Cancer. 2021 Oct;9(10). doi: 10.1136/jitc-2021-002989.
PURPOSE
Immune checkpoint inhibition (ICI) therapy has improved patient outcomes in advanced non-small cell lung cancer (NSCLC), but better biomarkers are needed. A clinically validated, blood-based proteomic test, or host immune classifier (HIC), was assessed for its ability to predict ICI therapy outcomes in this real-world, prospectively designed, observational study.
MATERIALS AND METHODS
The prospectively designed, observational registry study INSIGHT (Clinical Effectiveness Assessment of VeriStrat® Testing and Validation of Immunotherapy Tests in NSCLC Subjects) (NCT03289780) includes 35 US sites having enrolled over 3570 NSCLC patients at any stage and line of therapy. After enrolment and prior to therapy initiation, all patients are tested and designated HIC-Hot (HIC-H) or HIC-Cold (HIC-C). A prespecified interim analysis was performed after 1-year follow-up with the first 2000 enrolled patients. We report the overall survival (OS) of patients with advanced stage (IIIB and IV) NSCLC treated in the first-line (ICI-containing therapies n=284; all first-line therapies n=877), by treatment type and in HIC-defined subgroups.
RESULTS
OS for HIC-H patients was longer than OS for HIC-C patients across treatment regimens, including ICI. For patients treated with all ICI regimens, median OS was not reached (95% CI 15.4 to undefined months) for HIC-H (n=196) vs 5.0 months (95% CI 2.9 to 6.4) for HIC-C patients (n=88); HR=0.38 (95% CI 0.27 to 0.53), p<0.0001. For ICI monotherapy, OS was 16.8 vs 2.8 months (HR=0.36 (95% CI 0.22 to 0.58), p<0.0001) and for ICI with chemotherapy OS was unreached vs 6.4 months (HR=0.41 (95% CI 0.26 to 0.67), p=0.0003). HIC results were independent of programmed death ligand 1 (PD-L1). In a subgroup with PD-L1 ≥50% and performance status 0-1, HIC stratified survival significantly for ICI monotherapy but not ICI with chemotherapy.
CONCLUSION
Blood-based HIC proteomic testing provides clinically meaningful information for immunotherapy treatment decision in NSCLC independent of PD-L1. The data suggest that HIC-C patients should not be treated with ICI alone regardless of their PD-L1 expression.
目的
免疫检查点抑制(ICI)疗法改善了晚期非小细胞肺癌(NSCLC)患者的预后,但仍需要更好的生物标志物。本研究采用经过临床验证的、基于血液的蛋白质组学检测或宿主免疫分类器(HIC),评估其在这项真实世界、前瞻性设计、观察性研究中预测 ICI 治疗结果的能力。
材料和方法
前瞻性设计的观察性注册研究 INSIGHT(Veristrat® 检测的临床效果评估和 NSCLC 受试者免疫治疗检测的验证)(NCT03289780)包括 35 个美国站点,在任何治疗阶段和线数中入组了超过 3570 例 NSCLC 患者。入组后且在开始治疗前,所有患者均接受检测并指定为 HIC-高热(HIC-H)或 HIC-低温(HIC-C)。对前 2000 名入组患者进行了为期 1 年的随访后的预先指定的中期分析。我们报告了接受一线治疗(含 ICI 的治疗方案 n=284;所有一线治疗方案 n=877)的晚期(IIIB 和 IV 期)NSCLC 患者的总生存期(OS),按治疗类型和 HIC 定义的亚组进行报告。
结果
在包括 ICI 在内的各种治疗方案中,HIC-H 患者的 OS 长于 HIC-C 患者。接受所有 ICI 方案治疗的患者中,HIC-H 患者(n=196)的中位 OS 未达到(95%CI 15.4 至未定义的月份),而 HIC-C 患者(n=88)的中位 OS 为 5.0 个月(95%CI 2.9 至 6.4);HR=0.38(95%CI 0.27 至 0.53),p<0.0001。ICI 单药治疗的 OS 为 16.8 个月 vs 2.8 个月(HR=0.36(95%CI 0.22 至 0.58),p<0.0001),ICI 联合化疗的 OS 未达到 vs 6.4 个月(HR=0.41(95%CI 0.26 至 0.67),p=0.0003)。HIC 结果独立于程序性死亡配体 1(PD-L1)。在 PD-L1≥50%和表现状态 0-1 的亚组中,HIC 分层对 ICI 单药治疗具有显著的生存意义,但对 ICI 联合化疗无意义。
结论
基于血液的 HIC 蛋白质组学检测为 NSCLC 的免疫治疗决策提供了有临床意义的信息,独立于 PD-L1。数据表明,无论 PD-L1 表达如何,HIC-C 患者不应单独接受 ICI 治疗。
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