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Analysis of PD1, PDL1, PDL2 expression and T cells infiltration in 1014 gastric cancer patients

机译:1014例胃癌患者PD1,PDL1,PDL2表达和T细胞浸润的分析

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Although immune checkpoint blockade have demonstrated promising results, their effects on gastric cancer (GC) are under investigation. Understanding the clinical significance of PD1 and its ligands' expression, together with T cell infiltration might provide clues for biomarkers screening in GC immunotherapy. Immunohistochemistry were performed on a tissue microarray including 1,014 GC specimens using PD1, PDL1 and PDL2 antibodies. T cell markers CD3 and CD8 were also stained and quantified by automated image analysis. Correlation with clinical features and outcome were analyzed after controlling for potential confounders including EBV infection, HER2, C-met and PCNA expression. 37.8% of the cases showed membranous PD-L1 expression in tumor cells and 74.9% in infiltrating immune cells. PDL1 expression rate was rather higher in patients without metastasis, in EBV positive group and those with C-met and PCNA expression. GC patients with high level PDL1 expression exhibited better survival. GC Patients with higher T cell infiltration also showed elevated PDL1, PDL2 and PD1 expression and predict favorable outcome, indicating an adaptive immune resistance mechanism may exist. The group of patients infiltrated with lower density CD3+ T cells also without PDL1 expression in tumor cells predict the worst outcome in the subgroup of different PTNM stage, which may suggest an inactive immune status. These results highlights the need to assess both PDL1 expression in all tumor context and the characterization of the GC immune microenvironment.
机译:虽然免疫检查点延迟已经证明了有希望的结果,但它们对胃癌(GC)的影响是正在调查的。了解PD1及其配体表达的临床意义,与T细胞浸润一起,可以为GC免疫疗法筛选生物标志物筛选的线索。在包括使用PD1,PDL1和PDL2抗体的组织微阵列上进行免疫组织化学。 T细胞标记物CD3和CD8也通过自动图像分析染色和量化。在控制潜在的混凝剂后,分析了与临床特征和结果的相关性,包括EBV感染,HER2,C-Met和PCNA表达。 37.8%的病例在肿瘤细胞中显示出膜质PD-L1表达,渗透免疫细胞74.9%。在没有转移的患者中,在eBV阳性组和具有C-Met和PCNA表达的患者中,PDL1表达率相当较高。高水平PDL1表达的GC患者表现出更好的存活率。具有较高T细胞浸润的GC患者也显示出PDL1,PDL2和PD1表达升高,并且预测有利的结果,表明可以存在适应性免疫抵抗机制。患有较低密度CD3 + T细胞的患者的患者也没有PDL1在肿瘤细胞中的表达预测不同PTNM阶段的亚组中最糟糕的结果,这可能表明免疫的免疫状态。这些结果突出了在所有肿瘤上下文中评估PDL1表达的需要以及GC免疫微环境的表征。

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