Identifying epithelial-mesenchymal transition-related genes as prognostic biomarkers and therapeutic targets of hepatocellular carcinoma by integrated analysis of single-cell and bulk-RNA sequencing data.

IF 1.5 4区医学 Q4 ONCOLOGY

Translational cancer research Pub Date : 2024-08-31 Epub Date: 2024-08-22 DOI:10.21037/tcr-24-521

Chen Chen, Shunyi Wang, Yuhong Tang, Huanxiang Liu, Daoyuan Tu, Bingbing Su, Rui Peng, Shengjie Jin, Guoqing Jiang, Jun Cao, Chi Zhang, Dousheng Bai

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引用次数: 0

Abstract

Background: Hepatocellular carcinoma (HCC) remains one of the most lethal cancers globally. Patients with advanced HCC tend to have poor prognoses and shortened survival. Recently, data from bulk RNA sequencing have been employed to discover prognostic markers for various cancers. However, they fall short in precisely identifying core molecular and cellular activities within tumor cells. In our present study, we combined bulk-RNA sequencing (bulk RNA-seq) data with single-cell RNA sequencing (scRNA-seq) to develop a prognostic model for HCC. The goal of our research is to uncover new biomarkers and enhance the accuracy of HCC prognosis prediction.

Methods: Integrating single-cell sequencing data with transcriptomics were used to identify epithelial-mesenchymal transition (EMT)-related genes (ERGs) implicated in HCC progression and their clinical significance was elucidated. Utilizing marker genes derived from core cells and ERGs, we constructed a prognostic model using univariate Cox analysis, exploring a multitude of algorithmic combinations, and further refining it through multivariate Cox analysis. Additionally, we conducted an in-depth investigation into the disparities in clinicopathological features, immune microenvironment composition, immune checkpoint expression, and chemotherapeutic drug sensitivity profiles between high- and low-risk patient cohorts.

Results: We developed a prognostic model predicated on the expression profiles of eight signature genes, namely HSP90AA1, CIRBP, CCR7, S100A9, ADAM17, ENG, PGF, and INPP4B, aiming at predicting overall survival (OS) outcomes. Notably, patients classified with high-risk scores exhibited a propensity towards diminished OS rates, heightened frequencies of stage III-IV disease, increased tumor mutational burden (TMB), augmented immune cell infiltration, and diminished responsiveness to immunotherapeutic interventions.

Conclusions: This study presented a novel prognostic model for predicting the survival of HCC patients by integrating scRNA-seq and bulk RNA-seq data. The risk score emerges as a promising independent prognostic factor, showing a correlation with the immune microenvironment and clinicopathological features. It provided new clinical tools for predicting prognosis and aided future research into the pathogenesis of HCC.

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通过综合分析单细胞和大量 RNA 测序数据，确定作为肝细胞癌预后生物标志物和治疗靶点的上皮-间质转化相关基因。

背景：肝细胞癌（HCC）仍然是全球致死率最高的癌症之一。晚期肝细胞癌患者往往预后不良，生存期缩短。最近，大量 RNA 测序数据被用来发现各种癌症的预后标志物。然而，它们在精确识别肿瘤细胞内的核心分子和细胞活动方面存在不足。在本研究中，我们将批量 RNA 测序（bulk RNA-seq）数据与单细胞 RNA 测序（scRNA-seq）结合起来，建立了一个 HCC 的预后模型。我们的研究目标是发现新的生物标志物，提高HCC预后预测的准确性：方法：将单细胞测序数据与转录组学相结合，鉴定与HCC进展有关的上皮-间质转化（EMT）相关基因（ERGs），并阐明其临床意义。利用从核心细胞和 ERGs 提取的标记基因，我们通过单变量 Cox 分析构建了一个预后模型，探索了多种算法组合，并通过多变量 Cox 分析进一步完善了该模型。此外，我们还深入研究了高危和低危患者队列在临床病理特征、免疫微环境组成、免疫检查点表达和化疗药物敏感性方面的差异：我们根据8个特征基因（即HSP90AA1、CIRBP、CCR7、S100A9、ADAM17、ENG、PGF和INPP4B）的表达谱建立了一个预后模型，旨在预测总生存期（OS）结果。值得注意的是，被归入高风险评分的患者表现出OS率降低、III-IV期疾病发生率增加、肿瘤突变负荷（TMB）增加、免疫细胞浸润增加以及对免疫治疗干预反应性降低的倾向：本研究通过整合 scRNA-seq 和大量 RNA-seq 数据，提出了一种预测 HCC 患者生存期的新型预后模型。风险评分是一个有前景的独立预后因素，与免疫微环境和临床病理特征相关。它为预测预后提供了新的临床工具，并有助于未来对 HCC 发病机制的研究。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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来源期刊

Translational cancer research ONCOLOGY-

CiteScore

2.10

自引率

0.00%

发文量

252

期刊介绍： Translational Cancer Research (Transl Cancer Res TCR; Print ISSN: 2218-676X; Online ISSN 2219-6803; http://tcr.amegroups.com/) is an Open Access, peer-reviewed journal, indexed in Science Citation Index Expanded (SCIE). TCR publishes laboratory studies of novel therapeutic interventions as well as clinical trials which evaluate new treatment paradigms for cancer; results of novel research investigations which bridge the laboratory and clinical settings including risk assessment, cellular and molecular characterization, prevention, detection, diagnosis and treatment of human cancers with the overall goal of improving the clinical care of cancer patients. The focus of TCR is original, peer-reviewed, science-based research that successfully advances clinical medicine toward the goal of improving patients'' quality of life. The editors and an international advisory group of scientists and clinician-scientists as well as other experts will hold TCR articles to the high-quality standards. We accept Original Articles as well as Review Articles, Editorials and Brief Articles.