Identification and Validation of Cytotoxicity-Related Features to Predict Prognostic and Immunotherapy Response in Patients with Clear Cell Renal Cell Carcinoma.

IF 1.4 4区 生物学 Q4 GENETICS & HEREDITY
Genetics research Pub Date : 2024-08-30 eCollection Date: 2024-01-01 DOI:10.1155/2024/3468209
Junxiao Yu, Bowen Zhao, You Yu
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引用次数: 0

Abstract

Background: Clear cell renal cell carcinoma (ccRCC) is a renal cortical malignancy with a complex pathogenesis. Identifying ideal biomarkers to establish more accurate promising prognostic models is crucial for the survival of kidney cancer patients.

Methods: Seurat R package was used for single-cell RNA-sequencing (scRNA-seq) data filtering, dimensionality reduction, clustering, and differentially expressed genes analysis. Gene coexpression network analysis (WGCNA) was performed to identify the cytotoxicity-related module. The independent cytotoxicity-related risk model was established by the survival R package, and Kaplan-Meier (KM) survival analysis and timeROC with area under the curve (AUC) were employed to confirm the prognosis and effectiveness of the risk model. The risk and prognosis in patients suffering from ccRCC were predicted by establishing a nomogram. A comparison of the level of immune infiltration in different risk groups and subtypes using the CIBERSORT, MCP-counter, and TIMER methods, as well as assessment of drug sensitivity to conventional chemotherapeutic agents in risk groups using the pRRophetic package, was made.

Results: Eleven ccRCC subpopulations were identified by single-cell sequencing data from the GSE224630 dataset. The identified cytotoxicity-related T-cell cluster and module genes defined three cytotoxicity-related molecular subtypes. Six key genes (SOWAHB, SLC16A12, IL20RB, SLC12A8, PLG, and HHLA2) affecting prognosis risk genes were selected for developing a risk model. A nomogram containing the RiskScore and stage revealed that the RiskScore contributed the most and exhibited excellent predicted performance for prognosis in the calibration plots and decision curve analysis (DCA). Notably, high-risk patients with ccRCC demonstrate a poorer prognosis with higher immune infiltration characteristics and TIDE scores, whereas low-risk patients are more likely to benefit from immunotherapy.

Conclusions: A ccRCC survival prognostic model was produced based on the cytotoxicity-related signature, which had important clinical significance and may provide guidance for ccRCC treatment.

识别和验证细胞毒性相关特征以预测透明细胞肾细胞癌患者的预后和免疫治疗反应
背景:透明细胞肾细胞癌(ccRCC)是一种发病机制复杂的肾皮质恶性肿瘤。确定理想的生物标志物以建立更准确、更有前景的预后模型对肾癌患者的生存至关重要:方法:使用 Seurat R 软件包进行单细胞 RNA 序列(scRNA-seq)数据过滤、降维、聚类和差异表达基因分析。基因共表达网络分析(WGCNA)用于识别细胞毒性相关模块。利用生存R软件包建立了独立的细胞毒性相关风险模型,并采用Kaplan-Meier(KM)生存分析和带曲线下面积(AUC)的时间ROC来确认风险模型的预后和有效性。通过建立提名图,预测了ccRCC患者的风险和预后。使用CIBERSORT、MCP-counter和TIMER方法比较了不同风险组和亚型的免疫浸润水平,并使用pRRophetic软件包评估了风险组对常规化疗药物的敏感性:结果:通过 GSE224630 数据集中的单细胞测序数据确定了 11 个 ccRCC 亚群。确定的细胞毒性相关 T 细胞群和模块基因定义了三种细胞毒性相关分子亚型。研究人员选择了影响预后风险基因的六个关键基因(SOWAHB、SLC16A12、IL20RB、SLC12A8、PLG 和 HHLA2)来建立风险模型。包含 RiskScore 和分期的提名图显示,RiskScore 的贡献最大,在校准图和决策曲线分析(DCA)中表现出卓越的预后预测性能。值得注意的是,高危ccRCC患者的预后较差,免疫浸润特征和TIDE评分较高,而低危患者更有可能从免疫疗法中获益:结论:基于细胞毒性相关特征建立的ccRCC生存预后模型具有重要的临床意义,可为ccRCC治疗提供指导。
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来源期刊
Genetics research
Genetics research 生物-遗传学
自引率
6.70%
发文量
74
审稿时长
>12 weeks
期刊介绍: Genetics Research is a key forum for original research on all aspects of human and animal genetics, reporting key findings on genomes, genes, mutations and molecular interactions, extending out to developmental, evolutionary, and population genetics as well as ethical, legal and social aspects. Our aim is to lead to a better understanding of genetic processes in health and disease. The journal focuses on the use of new technologies, such as next generation sequencing together with bioinformatics analysis, to produce increasingly detailed views of how genes function in tissues and how these genes perform, individually or collectively, in normal development and disease aetiology. The journal publishes original work, review articles, short papers, computational studies, and novel methods and techniques in research covering humans and well-established genetic organisms. Key subject areas include medical genetics, genomics, human evolutionary and population genetics, bioinformatics, genetics of complex traits, molecular and developmental genetics, Evo-Devo, quantitative and statistical genetics, behavioural genetics and environmental genetics. The breadth and quality of research make the journal an invaluable resource for medical geneticists, molecular biologists, bioinformaticians and researchers involved in genetic basis of diseases, evolutionary and developmental studies.
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