Prognostic immune markers in esophageal cancer patients managed with trimodal therapy.

IF 4.6 2区医学 Q2 IMMUNOLOGY Cancer Immunology, Immunotherapy Pub Date : 2025-01-03 DOI:10.1007/s00262-024-03891-3

Mark K Farrugia, Elizabeth A Repasky, Minhui Chen, Kristopher Attwood, Kayla Catalfamo, Hanna Rosenheck, Song Yao, David M Mattson, Sarbajit Mukherjee, Moshim Kukar, Agnieszka K Witkiewicz, Anurag K Singh

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Abstract

Background: Esophageal cancer (ESC) is an aggressive disease which often presents at an advanced stage. Despite trimodal therapy, 40-50% patients can develop metastatic disease by 18 months. Identification of patients at risk for metastatic spread is challenging with need for improved prognostication. We investigated whether the immune landscape of pretreatment tissue was associated with relapse in ESC patients.

Methods: Between April 2010 and October 2018, we identified 25 patients who had undergone trimodal therapy for ESC and had pretreatment biopsies suitable for analyses. We performed high-throughput multispectral immunofluorescence (mIF) analysis on formalin-fixed paraffin embedded biopsy samples. Analysis of 27 unique populations via immune and exhaustion mIF panels was performed and expression was normalized to total cell counts.

Results: Of the 25 patients analyzed, the median follow-up time was 23.9 months, during which 12 (48%) patients suffered a relapse with a median time to progression of 13.1 months. mIF revealed higher expression of HLA-DR (p = 0.019), CD8/LAG3 (p = 0.046), and CD8/CTLA4 (p = 0.027) among patients without relapse. Time to progression (TTP) and disease-specific survival (DSS) were stratified by median expression of each significant subpopulation and formally tested by the log-rank test. Higher than median expression of HLA-DR (p = 0.027), CD8/LAG3 (p = 0.039), and CD8/CTLA4 (p = 0.039) were significantly associated with TTP. Similarly, HLA-DR (p = 0.0069) and CD8/CTLA4 (p = 0.036) were significantly associated with improved DSS, whereas no significant observations were found with CD8/LAG3 (p = 0.11) expression. Stromal, but not tumoral expression of CD163 and CD163/PDL1 were significantly associated with improved TTP and DSS.

Conclusions: High expression of HLA-DR, CD8/CTLA4, and stromal expression of CD163 and CD163/PDL1 within pretreatment biopsy ESC samples was associated with significantly reduced rates of relapse. Increased presence of these markers suggests that an improved immune landscape is associated with less aggressive disease and may provide an opportunity for risk-based treatment strategies.

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食管癌患者经三模式治疗后的预后免疫标记物

背景：食管癌（ESC）是一种侵袭性疾病，通常处于晚期。尽管采用了三联疗法，但仍有 40-50% 的患者会在 18 个月内出现转移性疾病。鉴别有转移风险的患者具有挑战性，需要改善预后。我们研究了治疗前组织的免疫景观是否与 ESC 患者的复发有关：2010年4月至2018年10月期间，我们确定了25名接受过ESC三联疗法的患者，他们的治疗前活检组织适合进行分析。我们对福尔马林固定石蜡包埋活检样本进行了高通量多谱段免疫荧光（mIF）分析。我们通过免疫和衰竭 mIF 面板对 27 个独特的群体进行了分析，并将表达与细胞总数进行了归一化处理：mIF显示，未复发患者的HLA-DR（p = 0.019）、CD8/LAG3（p = 0.046）和CD8/CTLA4（p = 0.027）表达较高。进展时间（TTP）和疾病特异性生存期（DSS）根据各重要亚群的中位表达量进行分层，并通过对数秩检验进行正式检验。HLA-DR（p = 0.027）、CD8/LAG3（p = 0.039）和 CD8/CTLA4（p = 0.039）的表达高于中位数与 TTP 显著相关。同样，HLA-DR（p = 0.0069）和 CD8/CTLA4（p = 0.036）与 DSS 的改善明显相关，而 CD8/LAG3 （p = 0.11）的表达则无明显观察结果。CD163和CD163/PDL1的基质表达（而非肿瘤表达）与TTP和DSS的改善显著相关：结论：在预处理活检的 ESC 样本中，HLA-DR、CD8/CTLA4 的高表达以及 CD163 和 CD163/PDL1 的基质表达与复发率的显著降低有关。这些标志物的增加表明，免疫状况的改善与侵袭性较低的疾病有关，并为基于风险的治疗策略提供了机会。

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来源期刊

Cancer Immunology, Immunotherapy 医学-免疫学

CiteScore

10.50

自引率

1.70%

发文量

207

审稿时长

1 months

期刊介绍： Cancer Immunology, Immunotherapy has the basic aim of keeping readers informed of the latest research results in the fields of oncology and immunology. As knowledge expands, the scope of the journal has broadened to include more of the progress being made in the areas of biology concerned with biological response modifiers. This helps keep readers up to date on the latest advances in our understanding of tumor-host interactions. The journal publishes short editorials including "position papers," general reviews, original articles, and short communications, providing a forum for the most current experimental and clinical advances in tumor immunology.