Literature DB >> 29399387

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

Xiaofang Xing1, Jianping Guo2, Guangyu Ding1, Bo Li3, Bin Dong4, Qin Feng4, Shen Li5, Jian Zhang6, Xiaomin Ying6, Xiaojing Cheng1, Ting Guo1, Hong Du1, Ying Hu7, Tao Zhou8, Xiaohong Wang7, Lin Li1, Qingda Li1, Meng Xie1, Liting Li1, Xiangyu Gao1, Fei Shan5, Ziyu Li5, Xianzi Wen1, Jiping Wang9, Jiafu Ji1,4,5,7.   

Abstract

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.

Entities:  

Keywords:  PD1; PDL1; PDL2; T cells; gastric cancer; prognosis

Year:  2017        PMID: 29399387      PMCID: PMC5790386          DOI: 10.1080/2162402X.2017.1356144

Source DB:  PubMed          Journal:  Oncoimmunology        ISSN: 2162-4011            Impact factor:   8.110


  44 in total

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