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全面的基因组荟萃分析确定肿瘤内基质是预测胃癌患者生存的一个指标。

Comprehensive genomic meta-analysis identifies intra-tumoural stroma as a predictor of survival in patients with gastric cancer.

机构信息

Cellular and Molecular Research, National Cancer Centre, Singapore.

出版信息

Gut. 2013 Aug;62(8):1100-11. doi: 10.1136/gutjnl-2011-301373. Epub 2012 Jun 26.

DOI:10.1136/gutjnl-2011-301373
PMID:22735568
Abstract

OBJECTIVE

Gastric adenocarcinoma (gastric cancer, GC) is a major cause of global cancer mortality. Identifying molecular programmes contributing to GC patient survival may improve our understanding of GC pathogenesis, highlight new prognostic factors and reveal novel therapeutic targets. The authors aimed to produce a comprehensive inventory of gene expression programmes expressed in primary GCs, and to identify those expression programmes significantly associated with patient survival.

DESIGN

Using a network-modelling approach, the authors performed a large-scale meta-analysis of GC transcriptome data integrating 940 gastric transcriptomes from multiple independent patient cohorts. The authors analysed a training set of 428 GCs and 163 non-malignant gastric samples, and a validation set of 288 GCs and 61 non-malignant gastric samples.

RESULTS

The authors identified 178 gene expression programmes ('modules') expressed in primary GCs, which were associated with distinct biological processes, chromosomal location patterns, cis-regulatory motifs and clinicopathological parameters. Expression of a transforming growth factor β (TGF-β) signalling associated 'super-module' of stroma-related genes consistently predicted patient survival in multiple GC validation cohorts. The proportion of intra-tumoural stroma, quantified by morphometry in tissue sections from gastrectomy specimens, was also significantly associated with stromal super-module expression and GC patient survival.

CONCLUSION

Stromal gene expression predicts GC patient survival in multiple independent cohorts, and may be closely related to the intra-tumoural stroma proportion, a specific morphological GC phenotype. These findings suggest that therapeutic approaches targeting the GC stroma may merit evaluation.

摘要

目的

胃腺癌(胃癌,GC)是全球癌症死亡的主要原因。确定有助于 GC 患者生存的分子程序可能有助于我们更好地了解 GC 的发病机制,突出新的预后因素,并揭示新的治疗靶点。作者旨在制作一个在原发性 GC 中表达的基因表达程序的综合清单,并确定与患者生存显著相关的表达程序。

设计

作者使用网络建模方法对 GC 转录组数据进行了大规模的荟萃分析,整合了来自多个独立患者队列的 940 个胃转录组。作者分析了一个由 428 个 GC 和 163 个非恶性胃样本组成的训练集,以及一个由 288 个 GC 和 61 个非恶性胃样本组成的验证集。

结果

作者鉴定了 178 个在原发性 GC 中表达的基因表达程序(“模块”),这些程序与不同的生物学过程、染色体位置模式、顺式调控基序和临床病理参数相关。转化生长因子β(TGF-β)信号相关的“超级模块”的表达一致预测了多个 GC 验证队列中患者的生存情况。通过对胃切除术标本组织切片进行形态计量学定量的肿瘤内基质比例,也与基质超级模块表达和 GC 患者生存显著相关。

结论

基质基因表达在多个独立队列中预测 GC 患者的生存情况,并且可能与肿瘤内基质比例密切相关,这是一种特定的 GC 形态学表型。这些发现表明,靶向 GC 基质的治疗方法可能值得评估。

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