异常检测和人工智能发现弥漫大 B 细胞淋巴瘤中细胞凋亡和 RELB 原癌基因、NF-kB 亚基的致病作用

J. Carreras, R. Hamoudi
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引用次数: 0

摘要

背景:弥漫大 B 细胞淋巴瘤(DLBCL)是最常见的淋巴瘤之一。DLBCL在表型、基因和临床上都存在异质性。目的:我们旨在确定新的预后标志物。方法:进行异常检测分析:我们利用淋巴瘤/白血病分子谱分析项目(GSE10846)中 414 例患者的基因表达数据以及 10 例反应性扁桃体和 30 例 DLBCL 的免疫组化数据,进行了异常检测分析、其他人工智能技术和常规统计。研究结果首先,无监督异常检测分析找出了系列中的异常值(异常),并确定了 12 个基因:DPM2、TRAPPC1、HYAL2、TRIM35、NUDT18、TMEM219、CHCHD10、IGFBP7、LAMTOR2、ZNF688、UBL7和RELB,它们属于凋亡、MAPK、MTOR和NF-kB通路。其次,利用机器学习、人工神经网络和传统统计学方法预测这12个基因的总生存率。在多变量 Cox 回归分析中,HYAL2 和 UBL7 的高表达与总生存率差相关,而 TRAPPC1、IGFBP7 和 RELB 则与总生存率好相关(P < 0.01)。RELB作为单一标记物,仅在RCHOP类治疗病例中,其预后价值通过GSEA分析和Kaplan-Meier与对数秩检验得到了证实,并在TCGA和GSE57611数据集中得到了验证。异常检测分析在 GSE31312 和 GSE117556 数据集中得到了成功测试。通过免疫组化,RELB 在 B 淋巴细胞和巨噬细胞/树突状细胞中呈阳性,并探讨了其与 HLA DP-DR、SIRPA、CD85A (LILRB3)、PD-L1、MARCO 和 TOX 的相关性。结论异常检测和其他生物信息学技术成功地预测了DLBCL的预后,高RELB与良好的预后相关。
本文章由计算机程序翻译,如有差异,请以英文原文为准。
Anomaly Detection and Artificial Intelligence Identified the Pathogenic Role of Apoptosis and RELB Proto-Oncogene, NF-kB Subunit in Diffuse Large B-Cell Lymphoma
Background: Diffuse large B-cell lymphoma (DLBCL) is one of the most frequent lymphomas. DLBCL is phenotypically, genetically, and clinically heterogeneous. Aim: We aim to identify new prognostic markers. Methods: We performed anomaly detection analysis, other artificial intelligence techniques, and conventional statistics using gene expression data of 414 patients from the Lymphoma/Leukemia Molecular Profiling Project (GSE10846), and immunohistochemistry in 10 reactive tonsils and 30 DLBCL cases. Results: First, an unsupervised anomaly detection analysis pinpointed outliers (anomalies) in the series, and 12 genes were identified: DPM2, TRAPPC1, HYAL2, TRIM35, NUDT18, TMEM219, CHCHD10, IGFBP7, LAMTOR2, ZNF688, UBL7, and RELB, which belonged to the apoptosis, MAPK, MTOR, and NF-kB pathways. Second, these 12 genes were used to predict overall survival using machine learning, artificial neural networks, and conventional statistics. In a multivariate Cox regression analysis, high expressions of HYAL2 and UBL7 were correlated with poor overall survival, whereas TRAPPC1, IGFBP7, and RELB were correlated with good overall survival (p < 0.01). As a single marker and only in RCHOP-like treated cases, the prognostic value of RELB was confirmed using GSEA analysis and Kaplan–Meier with log-rank test and validated in the TCGA and GSE57611 datasets. Anomaly detection analysis was successfully tested in the GSE31312 and GSE117556 datasets. Using immunohistochemistry, RELB was positive in B-lymphocytes and macrophage/dendritic-like cells, and correlation with HLA DP-DR, SIRPA, CD85A (LILRB3), PD-L1, MARCO, and TOX was explored. Conclusions: Anomaly detection and other bioinformatic techniques successfully predicted the prognosis of DLBCL, and high RELB was associated with a favorable prognosis.
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