非鳞状和鳞状 NSCLC 中有害 LRP1B 基因突变对预测免疫检查点抑制剂单独使用或与化疗联合使用对化疗单独使用的益处的反作用:POPLAR/OAK 和 CHOICE-01 试验的回顾性分析。

IF 8 2区 生物学 Q1 BIOLOGY
Jinliang Wang, Wenyong Zhou, Yu Xu, Jianchun Duan, Qiaoxia Zhou, Guoqiang Wang, Leo Li, Chunwei Xu, Wenxian Wang, Shangli Cai, Zhijie Wang, Jie Wang
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引用次数: 0

摘要

在非小细胞肺癌中,非鳞癌亚型和鳞癌亚型(nsqNSCLC和sqNSCLC)在病理生理学、肿瘤免疫学和影响免疫检查点抑制剂(ICI)治疗反应的潜在基因组相关性方面表现出差异。在我们的内部训练队列(n=85)中,在nsqNSCLCs和sqNSCLCs中,LRP1B有害突变(LRP1B-del)的存在分别与单用ICIs的无进展生存期(PFS)的延长和缩短有关(Pinteraction=0.008)。这些结果在一个更大的公共 ICI 队列中得到了验证(n=208,Pinteraction+ T 细胞分别在 nsqNSCLCs(P=0.040)和 sqNSCLCs(P=0.014)中得到了验证。在POPLAR/OAK队列中,有LRP1B-del的nsqNSCLC比多西他赛更能从atezolizumab中获益(危险比(HR)=0.70,P=0.046),而没有LRP1B-del的nsqNSCLC的获益则微乎其微(HR=1.05,P=0.64)。相反,无LRP1B-del的sqNSCLC比有LRP1B-del的sqNSCLC更能从阿特珠单抗中获益(HR=0.60,P=0.002)(HR=1.30,P=0.31)。在内部的CHOICE-01队列中也观察到了一致的结果,有LRP1B-del的nsqNSCLCs和没有LRP1B-del的sqNSCLCs从托瑞帕利单抗联合化疗中获益比从单独化疗中获益更多(Pinteraction=0.008)。这项多队列研究阐明了LRP1B-del在nsqNSCLCs和sqNSCLCs中对预测单用ICI或联合化疗比单用化疗获益的反作用。我们的研究结果凸显了 LRP1B-del 在指导 nsqNSCLCs 和 sqNSCLCs 治疗选择方面的不同临床效用,强调了在研究癌症治疗生物标记物时根据病理亚型进行详细分析的必要性。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Antithetical impacts of deleterious LRP1B mutations in non-squamous and squamous NSCLCs on predicting benefits from immune checkpoint inhibitor alone or with chemotherapy over chemotherapy alone: retrospective analyses of the POPLAR/OAK and CHOICE-01 trials.

In non-small cell lung cancers, the non-squamous and squamous subtypes (nsqNSCLC and sqNSCLC) exhibit disparities in pathophysiology, tumor immunology, and potential genomic correlates affecting responses to immune checkpoint inhibitor (ICI)-based treatments. In our in-house training cohort (n=85), the presence of the LRP1B deleterious mutation (LRP1B-del) was associated with longer and shorter progression-free survival (PFS) on ICIs alone in nsqNSCLCs and sqNSCLCs, respectively (Pinteraction=0.008). These results were validated using a larger public ICI cohort (n=208, Pinteraction<0.001). Multiplex immunofluorescence staining revealed an association between LRP1B-del and increased and decreased numbers of tumor-infiltrating CD8+ T cells in nsqNSCLCs (P=0.040) and sqNSCLCs (P=0.014), respectively. In the POPLAR/OAK cohort, nsqNSCLCs with LRP1B-del demonstrated improved PFS benefits from atezolizumab over docetaxel (hazard ratio (HR) =0.70, P=0.046), whereas this benefit was negligible in those without LRP1B-del (HR=1.05, P=0.64). Conversely, sqNSCLCs without LRP1B-del benefited more from atezolizumab (HR=0.60, P=0.002) than those with LRP1B-del (HR=1.30, P=0.31). Consistent results were observed in the in-house CHOICE-01 cohort, in which nsqNSCLCs with LRP1B-del and sqNSCLCs without LRP1B-del benefited more from toripalimab plus chemotherapy than from chemotherapy alone (Pinteraction=0.008). This multi-cohort study delineates the antithetical impacts of LRP1B-del in nsqNSCLCs and sqNSCLCs on predicting the benefits from ICI alone or with chemotherapy over chemotherapy alone. Our findings highlight the distinct clinical utility of LRP1B-del in guiding treatment choices for nsqNSCLCs and sqNSCLCs, emphasizing the necessity for a detailed analysis based on pathological subtypes when investigating biomarkers for cancer therapeutics.

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来源期刊
CiteScore
15.10
自引率
8.80%
发文量
2907
审稿时长
3.2 months
期刊介绍: Science China Life Sciences is a scholarly journal co-sponsored by the Chinese Academy of Sciences and the National Natural Science Foundation of China, and it is published by Science China Press. The journal is dedicated to publishing high-quality, original research findings in both basic and applied life science research.
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