Development of a streamlined NGS-based TCGA classification scheme for gastric cancer and its implications for personalized therapy.

IF 2 4区 医学 Q3 GASTROENTEROLOGY & HEPATOLOGY Journal of gastrointestinal oncology Pub Date : 2024-10-31 Epub Date: 2024-09-13 DOI:10.21037/jgo-24-345
Pengda Guo, Yang Yang, Lu Wang, Yu Zhang, Bei Zhang, Jinping Cai, Fabrício Freire de Melo, Matthew R Strickland, Min Huang, Biao Liu
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Abstract

Background: The Cancer Genome Atlas (TCGA) has identified four distinct molecular subtypes of gastric cancer (GC) with prognostic significance: Epstein-Barr virus (EBV)-positive, microsatellite instability (MSI)-high, genomically stable (GS), and chromosomal instability (CIN). Unfortunately, the complex analysis required for TCGA classification limits its practical use in clinical settings. Our study sought to devise a next-generation sequencing (NGS)-based method to classify GC more efficiently, serving as a promising biomarker for prognosis and immunotherapy efficacy.

Methods: This study was a retrospective observation study, and we employed 2 independent GC cohorts. The 3DMed cohort (n=765), comprising data on 733 cancer-related genes along with 4 EBV-encoded genes, was utilized to develop the new NGS classification. Additionally, the secondary Korean cohort (n=55), which includes both genomic data and information on immune checkpoint inhibitor (ICI) treatment, was employed to establish a correlation between NGS subtypes and ICI responsiveness.

Results: In the 3DMed cohort, we identified 5.2% EBV, 4.6% MSI, 30.6% GS, and 59.6% CIN subtypes. The MSI subtype exhibited the highest number of mutation events, along with the highest tumor mutational burden (TMB) and strong programmed cell death ligand 1 (PD-L1) expression. CIN tumors showed extensive copy number variations (CNVs) and genomic heterogeneity. The EBV subtype presented recurrent ARID1A and PIK3CA mutations and fewer TP53 mutations. GS tumors exhibited specific mutations in CDH1 and ARID1A. In the Korean cohort, ICIs were most effective in MSI and EBV cases, showing disease control rates of 100%, compared to 62.9% in GS and 12.5% in CIN subtypes.

Conclusions: The NGS method successfully maps the mutational landscape of GC, providing a practical TCGA classification surrogate to optimize patient-specific treatment strategies.

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开发基于 NGS 的 TCGA 胃癌简化分类方案及其对个性化治疗的影响。
背景:癌症基因组图谱(TCGA)确定了胃癌(GC)具有预后意义的四种不同分子亚型:Epstein-Barr 病毒 (EBV) 阳性、微卫星不稳定性 (MSI) 高、基因组稳定 (GS) 和染色体不稳定性 (CIN)。遗憾的是,TCGA分类所需的复杂分析限制了其在临床环境中的实际应用。我们的研究试图设计一种基于下一代测序(NGS)的方法,更有效地对 GC 进行分类,作为预后和免疫疗法疗效的生物标志物:本研究是一项回顾性观察研究,我们采用了两个独立的 GC 队列。3DMed队列(n=765)包含733个癌症相关基因和4个EBV编码基因的数据,我们利用3DMed队列制定了新的NGS分类。此外,我们还采用了包含基因组数据和免疫检查点抑制剂(ICI)治疗信息的韩国二级队列(n=55)来建立 NGS 亚型与 ICI 反应性之间的相关性:在3DMed队列中,我们发现了5.2%的EBV亚型、4.6%的MSI亚型、30.6%的GS亚型和59.6%的CIN亚型。MSI亚型的突变事件数最多,肿瘤突变负荷(TMB)最高,程序性细胞死亡配体1(PD-L1)表达强。CIN肿瘤表现出广泛的拷贝数变异(CNV)和基因组异质性。EBV亚型中反复出现ARID1A和PIK3CA突变,TP53突变较少。GS肿瘤表现出CDH1和ARID1A的特异性突变。在韩国队列中,ICIs对MSI和EBV病例最为有效,疾病控制率达到100%,而GS和CIN亚型的疾病控制率分别为62.9%和12.5%:NGS方法成功绘制了GC的突变图谱,为优化患者特异性治疗策略提供了实用的TCGA分类替代物。
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来源期刊
CiteScore
3.20
自引率
0.00%
发文量
171
期刊介绍: ournal of Gastrointestinal Oncology (Print ISSN 2078-6891; Online ISSN 2219-679X; J Gastrointest Oncol; JGO), the official journal of Society for Gastrointestinal Oncology (SGO), is an open-access, international peer-reviewed journal. It is published quarterly (Sep. 2010- Dec. 2013), bimonthly (Feb. 2014 -) and openly distributed worldwide. JGO publishes manuscripts that focus on updated and practical information about diagnosis, prevention and clinical investigations of gastrointestinal cancer treatment. Specific areas of interest include, but not limited to, multimodality therapy, markers, imaging and tumor biology.
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