诱导共刺激分子(ICOS)及其配体:肿瘤患者中的表达模式与结果
ICOS and ICOS ligand: expression patterns and outcomes in oncology patients.
作者信息
Nikanjam Mina, Kato Shumei, Nishizaki Daisuke, Barkauskas Donald A, Pabla Sarabjot, Nesline Mary K, Conroy Jeffrey M, Naing Aung, Kurzrock Razelle
机构信息
Division of Hematology-Oncology, University of California San Diego, 1200 Garden View Road, La Jolla, CA 92024, USA.
Division of Hematology-Oncology, University of California San Diego, La Jolla, CA, USA.
出版信息
Ther Adv Med Oncol. 2025 Apr 24;17:17588359251330514. doi: 10.1177/17588359251330514. eCollection 2025.
BACKGROUND
Inducible T-cell co-stimulator (ICOS) and its ligand (ICOSL) form a complex, two-faced immune machinery that can lead to both immune stimulation and inhibition.
OBJECTIVE
We explored ICOS transcriptomic expression patterns and their relationship with other checkpoints and with outcomes in patients with advanced/metastatic cancers.
DESIGN
This was a retrospective cohort study.
METHODS
RNA expression for ICOS and other immune checkpoints was quantified by RNA sequencing and stratified by rank values into high (75-100 percentiles) and low (0-24 percentiles). Fischer's exact tests were used for univariate analyses to evaluate independent predictors of ICOS high and logistic regression was used for multivariate analyses. Progression-free survival (PFS) and overall survival (OS) for ICOS high versus not high expression were evaluated using the log-rank test (Kaplan-Meier analysis) and Cox proportional hazards.
RESULTS
High ICOS (⩾75 percentile RNA rank) was present in 14% of 514 cancers and independently associated with high PD-1 ( = 0.025), PD-L1 ( < 0.0001), and CTLA-4 RNA expression ( < 0.0001) and with patients not having colorectal cancer ( = 0.0009; multivariate analysis). Patterns of ICOS and ICOSL expression varied between and within tumor types. For 217 patients receiving immune checkpoint inhibitors (ICIs), there were no significant differences in PFS or OS between patients with ICOS high versus not-high expression (multivariate analysis). In 272 immunotherapy-naïve patients, OS was also similar between patients with ICOS high versus not-high expression ( = 0.91).
CONCLUSION
High ICOS expression was not a prognostic marker and did not independently predict outcomes after ICIs. Variable expression of ICOS/ICOSL between tumors and association of high ICOS with high PD-1, PD-L1, and CTLA-4 suggest that individual tumor immunomic analysis may be required for optimized patient selection in clinical trials targeting the ICOS/ICOSL system, especially when given in combination with ICIs.
TRIAL REGISTRATION
UCSD_PREDICT, NCT02478931.
背景
诱导性T细胞共刺激分子(ICOS)及其配体(ICOSL)形成一种复杂的、具有两面性的免疫机制,可导致免疫刺激和抑制。
目的
我们探讨了ICOS的转录组表达模式及其与其他检查点以及晚期/转移性癌症患者预后的关系。
设计
这是一项回顾性队列研究。
方法
通过RNA测序对ICOS和其他免疫检查点的RNA表达进行定量,并按秩值分层为高(第75 - 100百分位数)和低(第0 - 24百分位数)。采用Fisher精确检验进行单变量分析,以评估ICOS高表达的独立预测因素,采用逻辑回归进行多变量分析。使用对数秩检验(Kaplan - Meier分析)和Cox比例风险模型评估ICOS高表达与非高表达患者的无进展生存期(PFS)和总生存期(OS)。
结果
在514例癌症患者中,14%存在高ICOS(RNA秩⩾75百分位数),且与高PD - 1(P = 0.025)、PD - L1(P < 0.0001)和CTLA - 4 RNA表达(P < 0.0001)以及非结直肠癌患者独立相关(P = 0.0009;多变量分析)。ICOS和ICOSL的表达模式在肿瘤类型之间和内部存在差异。对于217例接受免疫检查点抑制剂(ICI)治疗的患者,ICOS高表达与非高表达患者的PFS或OS无显著差异(多变量分析)。在272例未接受过免疫治疗的患者中,ICOS高表达与非高表达患者的OS也相似(P = 0.91)。
结论
高ICOS表达不是一个预后标志物,也不能独立预测ICI治疗后的预后。肿瘤之间ICOS/ICOSL的可变表达以及高ICOS与高PD - 1、PD - L1和CTLA - 4的关联表明,在针对ICOS/ICOSL系统的临床试验中,可能需要进行个体肿瘤免疫组学分析以优化患者选择,特别是在与ICI联合使用时。
试验注册
UCSD_PREDICT,NCT02478931。
Zotero 插件