Validation of the prognostic value of CD3 and CD8 cell densities analogous to the Immunoscore® by stage and location of colorectal cancer: an independent patient cohort study

IF 3.4 2区 医学 Q1 PATHOLOGY
Elizabeth Alwers, Jakob N Kather, Matthias Kloor, Alexander Brobeil, Katrin E Tagscherer, Wilfried Roth, Amelie Echle, Efrat L Amitay, Jenny Chang-Claude, Hermann Brenner, Michael Hoffmeister
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引用次数: 1

Abstract

In addition to the traditional staging system in colorectal cancer (CRC), the Immunoscore® has been proposed to characterize the level of immune infiltration in tumor tissue and as a potential prognostic marker. The aim of this study was to examine and validate associations of an immune cell score analogous to the Immunoscore® with established molecular tumor markers and with CRC patient survival in a routine setting. Patients from a population-based cohort study with available CRC tumor tissue blocks were included in this analysis. CD3+ and CD8+ tumor infiltrating lymphocytes in the tumor center and invasive margin were determined in stained tumor tissue slides. Based on the T-cell density in each region, an  immune cell score closely analogous to the concept of the Immunoscore® was calculated and tumors categorized into IS-low, IS-intermediate, or IS-high. Logistic regression models were used to assess associations between clinicopathological characteristics with the immune cell score, and Cox proportional hazards models to analyze associations with cancer-specific, relapse-free, and overall survival. From 1,535 patients with CRC, 411 (27%) had IS-high tumors. Microsatellite instability (MSI-high) was strongly associated with higher immune cell score levels (p < 0.001). Stage I–III patients with IS-high had better CRC-specific and relapse-free survival compared to patients with IS-low (hazard ratio [HR] = 0.42 [0.27–0.66] and HR = 0.45 [0.31–0.67], respectively). Patients with microsatellite stable (MSS) tumors and IS-high had better survival (HRCSS = 0.60 [0.42–0.88]) compared to MSS/IS-low patients. In this population-based cohort of CRC patients, the immune cell score was significantly associated with better patient survival. It was a similarly strong prognostic marker in patients with MSI-high tumors and in the larger group of patients with MSS tumors. Additionally, this study showed that it is possible to implement an analogous immune cell score approach and validate the Immunoscore® using open source software in an academic setting. Thus, the Immunoscore® could be useful to improve the traditional staging system in colon and rectal cancer used in clinical practice.

Abstract Image

验证CD3和CD8细胞密度类似于Immunoscore®的结肠直肠癌分期和部位的预后价值:一项独立的患者队列研究
除了传统的结直肠癌(CRC)分期系统外,Immunoscore®已被提出用于表征肿瘤组织中的免疫浸润水平并作为潜在的预后标志物。本研究的目的是检查和验证免疫细胞评分(类似于Immunoscore®)与已建立的分子肿瘤标志物和CRC患者常规生存之间的关联。来自基于人群的队列研究的可用结直肠癌肿瘤组织块的患者被纳入该分析。染色肿瘤组织玻片检测肿瘤中心和浸润边缘的CD3+和CD8+肿瘤浸润淋巴细胞。根据每个区域的t细胞密度,计算与Immunoscore®概念非常相似的免疫细胞评分,并将肿瘤分类为IS-low, IS-intermediate或IS-high。使用Logistic回归模型来评估临床病理特征与免疫细胞评分之间的关系,并使用Cox比例风险模型来分析与癌症特异性、无复发和总生存期的关系。在1535例结直肠癌患者中,411例(27%)为高is肿瘤。微卫星不稳定性(msi -高)与较高的免疫细胞评分水平密切相关(p < 0.001)。I-III期is -高患者比is -低患者有更好的crc特异性和无复发生存(风险比[HR] = 0.42[0.27-0.66]和HR = 0.45[0.31-0.67])。微卫星稳定(MSS)肿瘤且is -高的患者比MSS/ is -低的患者生存率更高(HRCSS = 0.60[0.42-0.88])。在这个以人群为基础的CRC患者队列中,免疫细胞评分与更好的患者生存率显著相关。在msi高肿瘤患者和更大的MSS肿瘤患者群体中,它同样是一个强有力的预后标志物。此外,本研究表明,可以在学术环境中使用开源软件实现类似的免疫细胞评分方法并验证免疫评分®。因此,Immunoscore®可用于临床实践中改进传统的结直肠癌分期系统。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
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来源期刊
Journal of Pathology Clinical Research
Journal of Pathology Clinical Research Medicine-Pathology and Forensic Medicine
CiteScore
7.40
自引率
2.40%
发文量
47
审稿时长
20 weeks
期刊介绍: The Journal of Pathology: Clinical Research and The Journal of Pathology serve as translational bridges between basic biomedical science and clinical medicine with particular emphasis on, but not restricted to, tissue based studies. The focus of The Journal of Pathology: Clinical Research is the publication of studies that illuminate the clinical relevance of research in the broad area of the study of disease. Appropriately powered and validated studies with novel diagnostic, prognostic and predictive significance, and biomarker discover and validation, will be welcomed. Studies with a predominantly mechanistic basis will be more appropriate for the companion Journal of Pathology.
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