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Literature DB >> 29147610

Host immune response index in gastric cancer identified by comprehensive analyses of tumor immunity.

Charny Park^1,2, Junhun Cho^1,3, Jeeyun Lee⁴, So Young Kang¹, Ji Yeong An⁵, Min Gew Choi⁵, Jun Ho Lee⁵, Tae Sung Sohn⁵, Jae Moon Bae⁵, Sung Kim⁵, Seung Tae Kim⁴, Se Hoon Park⁴, Joon Oh Park⁴, Won Ki Kang⁴, Insuk Sohn⁶, Sin Ho Jung⁶, Myung-Soo Kang^7,8, Kyoung-Mee Kim¹.

Abstract

Tumor infiltrating lymphocytes (TIL) in Epstein-Barr virus (EBV)-associated/microsatellite-unstable (MSI) gastric carcinomas (GC) constitute immune-active principal cellular components of tumor microenvironment and contribute to better prognosis. With the remarkable success of cancer immunotherapies, there is an urgent need for a comprehensive understanding of tumor-immune interactions in patients with GC in the context of host immune response. To identify GC subtype-specific immune response gene set, we tested differentially expressed genes for MSI and EBV+ GC subtypes in randomly selected test set (n = 278) in merged ACRG-SMC microarray and TCGA RNA sequencing data set. We identified Host ImmunE Response index (HIERÏ) consisting of 29 immune genes classifying GC patients into robust 3 groups with prognostic significance. Immune-high cluster 1 was enriched with PD-L1High/EBV+/MSI/TILHigh with the best clinical outcome while immune-low cluster 3 displayed worst outcome and exemplified with PD-L1Low/EBV-/MSS. The results were validated in the same cohort (n = 279) and independent cohort (n = 181) with RNA from formalin-fixed paraffin-embedded (FFPE) tissue. Unexpectedly, nearly half of GC in cluster 1 were EBV-/MSS and 10% of cluster 3 GC were EBV+/MSI GC patients, suggesting that in addition to EBV+/MSI GC subtypes, EBV-/MSS subtype also constitutes almost half of high immune cluster and would be a good candidate for immune checkpoint inhibitor therapy. In contrary, almost 10% of EBV+/MSI GC patients may not respond to immune checkpoint inhibitor therapy. Thus, our HIERÏ gene signature demonstrates the potential to subclassify tumor immunity levels, predict prognosis and help immunotherapeutic decisions.

Entities: Chemical Disease Species

Keywords: EBV; PD-L1; biomarker; gastric cancer; gene signature; immune response; prognosis; survival; tumor infiltrating lymphocyte

Year: 2017 PMID： 29147610 PMCID： PMC5674954 DOI： 10.1080/2162402X.2017.1356150

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

32 in total

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16 in total

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2. Expression of CD274 mRNA Measured by qRT-PCR Correlates With PD-L1 Immunohistochemistry in Gastric and Urothelial Carcinoma.

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Review 6. Recent Findings in the Regulation of Programmed Death Ligand 1 Expression.

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8. Four distinct immune microenvironment subtypes in gastric adenocarcinoma with special reference to microsatellite instability.

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9. The Transcriptomic Landscape of Gastric Cancer: Insights into Epstein-Barr Virus Infected and Microsatellite Unstable Tumors.

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10. Computational measurement of tumor immune microenvironment in gastric adenocarcinomas.

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Journal: Sci Rep Date: 2018-09-17 Impact factor: 4.379