免疫治疗治疗的非小细胞肺癌中 MYC 免疫组化和拷贝数增益的预测价值和分子相关性。
Predictive value and molecular correlates of MYC immunohistochemistry and copy number gain in non-small cell lung carcinomas treated with immunotherapy.
机构信息
Department of Laboratory Medicine and Pathology, Mayo Clinic, Rochester, MN, USA.
Department of Medical Oncology, Mayo Clinic, Rochester, MN, USA.
出版信息
Lung Cancer. 2024 Sep;195:107927. doi: 10.1016/j.lungcan.2024.107927. Epub 2024 Aug 10.
OBJECTIVES
Accurately predicting which patients diagnosed with non-small cell lung cancer (NSCLC) will respond to immunotherapy remains a clinical challenge. This study aims to determine the associations between MYC immunoreactivity, MYC copy number gain (CNG), driver mutations and survival following immunotherapy treatment, to provide insight into whether clinical MYC assessment may have predictive value.
MATERIALS AND METHODS
MYC copy number status was determined in 82 patients with NSCLC treated with immunotherapy, and MYC immunohistochemistry (IHC) was performed on 80 of these cases. MYC staining in ≥ 40 % of tumor cells was considered positive. Driver gene alterations, PD-L1 status and survival outcomes were assessed through retrospective chart review. Overall survival (OS) and progression free survival (PFS) were calculated from the date of immunotherapy initiation.
RESULTS
Nine (11 %) of 82 cases had MYC CNG and 56 (70 %) of the 80 immunostained cases were positive for MYC. MYC CNG was significantly associated with STK11 mutation (P=0.023), whereas positive MYC IHC was significantly associated with KRAS mutation (P=0.0076) and current/former smoking (P=0.0007). MYC CNG and positive MYC IHC were not significantly associated with each other (P=0.42), or with PD-L1 ≥ 1 % (MYC CNG: P=0.10; MYC IHC: P=0.09). Positive MYC IHC and PD-L1 ≥ 1 % were both significant predictors of OS (MYC: HR 2.7, 95 % CI 1.1-6.4, P=0.026; PD-L1: HR 0.33, 95 % CI 0.15-0.72, P=0.0055). MYC IHC positive/PD-L1 < 1 % cases had the shortest OS (median 230 versus 918 days, P=0.00069) and PFS (median 84 versus 254 days, P=0.0087). MYC CNG was not associated with OS or PFS.
CONCLUSION
We find that positive MYC IHC is an independent predictor of shorter OS after immunotherapy treatment, with MYC positive/PD-L1 < 1 % status predictive of particularly poor immunotherapy response. We identify positive MYC IHC as a feature of possible relevance to NSCLC treatment selection and of interest for future therapy development.
目的
准确预测哪些诊断为非小细胞肺癌(NSCLC)的患者对免疫疗法有反应仍然是一个临床挑战。本研究旨在确定 MYC 免疫反应、MYC 拷贝数增益(CNG)、驱动突变与免疫治疗后生存之间的关系,为临床评估 MYC 是否具有预测价值提供依据。
材料和方法
对 82 例接受免疫治疗的 NSCLC 患者进行 MYC 拷贝数状态检测,并对其中 80 例进行 MYC 免疫组化(IHC)检测。肿瘤细胞中≥40%的 MYC 染色为阳性。通过回顾性病历审查评估驱动基因突变、PD-L1 状态和生存结局。从免疫治疗开始之日起计算总生存期(OS)和无进展生存期(PFS)。
结果
82 例中有 9 例(11%)存在 MYC CNG,80 例免疫组化染色中有 56 例(70%)为 MYC 阳性。MYC CNG 与 STK11 突变显著相关(P=0.023),而阳性 MYC IHC 与 KRAS 突变显著相关(P=0.0076)和吸烟史(P=0.0007)。MYC CNG 和阳性 MYC IHC 之间无显著相关性(P=0.42),也与 PD-L1≥1%无显著相关性(MYC CNG:P=0.10;MYC IHC:P=0.09)。阳性 MYC IHC 和 PD-L1≥1%均为 OS 的显著预测因素(MYC:HR 2.7,95%CI 1.1-6.4,P=0.026;PD-L1:HR 0.33,95%CI 0.15-0.72,P=0.0055)。MYC IHC 阳性/PD-L1<1%病例的 OS 最短(中位值 230 天与 918 天,P=0.00069)和 PFS 最短(中位值 84 天与 254 天,P=0.0087)。MYC CNG 与 OS 或 PFS 无关。
结论
我们发现阳性 MYC IHC 是免疫治疗后 OS 较短的独立预测因素,MYC 阳性/PD-L1<1%状态提示免疫治疗反应较差。我们发现阳性 MYC IHC 是 NSCLC 治疗选择中可能具有相关性的特征,值得进一步研究开发。
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