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Signatures of tumour immunity distinguish Asian and non-Asian gastric adenocarcinomas

生物 基因签名 癌症 免疫组织化学 肿瘤科 CD8型 微阵列分析技术 内科学 免疫系统 免疫学 医学 基因表达 基因 遗传学
作者
Suling J. Lin,Johann A. Gagnon-Bartsch,Iain Beehuat Tan,Sophie Earle,Louise Ruff,Katherine Pettinger,Bauke Ylstra,Nicole C.T. van Grieken,Sun Young Rha,Hyun Cheol Chung,Ju–Seog Lee,Jae‐Ho Cheong,Sung Hoon Noh,Toru Aoyama,Yohei Miyagi,Akira Tsuburaya,Takaki Yoshikawa,Jaffer A. Ajani,Alex Boussioutas,Khay Guan Yeoh,Wei Peng Yong,Jimmy Bok Yan So,Jeeyun Lee,Won Ki Kang,Sung‐Hoon Kim,Yoichi Kameda,Tomio Arai,Axel zur Hausen,Terence P. Speed,Heike I. Grabsch,Patrick Tan
出处
期刊:Gut [BMJ]
卷期号:64 (11): 1721-1731 被引量:216
标识
DOI:10.1136/gutjnl-2014-308252
摘要

Objective

Differences in gastric cancer (GC) clinical outcomes between patients in Asian and non-Asian countries has been historically attributed to variability in clinical management. However, recent international Phase III trials suggest that even with standardised treatments, GC outcomes differ by geography. Here, we investigated gene expression differences between Asian and non-Asian GCs, and if these molecular differences might influence clinical outcome.

Design

We compared gene expression profiles of 1016 GCs from six Asian and three non-Asian GC cohorts, using a two-stage meta-analysis design and a novel biostatistical method (RUV-4) to adjust for technical variation between cohorts. We further validated our findings by computerised immunohistochemical analysis on two independent tissue microarray (TMA) cohorts from Asian and non-Asian localities (n=665).

Results

Gene signatures differentially expressed between Asians and non-Asian GCs were related to immune function and inflammation. Non-Asian GCs were significantly enriched in signatures related to T-cell biology, including CTLA-4 signalling. Similarly, in the TMA cohorts, non-Asian GCs showed significantly higher expression of T-cell markers (CD3, CD45R0, CD8) and lower expression of the immunosuppressive T-regulatory cell marker FOXP3 compared to Asian GCs (p<0.05). Inflammatory cell markers CD66b and CD68 also exhibited significant cohort differences (p<0.05). Exploratory analyses revealed a significant relationship between tumour immunity factors, geographic locality-specific prognosis, and postchemotherapy outcomes.

Conclusions

Analyses of >1600 GCs suggest that Asian and non-Asian GCs exhibit distinct tumour immunity signatures related to T-cell function. These differences may influence geographical differences in clinical outcome, and the design of future trials particularly in immuno-oncology.
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