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Transcriptomic signatures of cellular and humoral immune responses in older adults after seasonal influenza vaccination identified by data-driven clustering

机译:通过数据驱动的聚类分析确定季节性流感疫苗接种后老年人的细胞和体液免疫反应的转录组学特征

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摘要

PBMC transcriptomes after influenza vaccination contain valuable information about factors affecting vaccine responses. However, distilling meaningful knowledge out of these complex datasets is often difficult and requires advanced data mining algorithms. We investigated the use of the data-driven Weighted Gene Correlation Network Analysis (WGCNA) gene clustering method to identify vaccine response-related genes in PBMC transcriptomic datasets collected from 138 healthy older adults (ages 50–74) before and after 2010–2011 seasonal trivalent influenza vaccination. WGCNA separated the 14,197 gene dataset into 15 gene clusters based on observed gene expression patterns across subjects. Eight clusters were strongly enriched for genes involved in specific immune cell types and processes, including B cells, T cells, monocytes, platelets, NK cells, cytotoxic T cells, and antiviral signaling. Examination of gene cluster membership identified signatures of cellular and humoral responses to seasonal influenza vaccination, as well as pre-existing cellular immunity. The results of this study illustrate the utility of this publically available analysis methodology and highlight genes previously associated with influenza vaccine responses (e.g., CAMK4, CD19), genes with functions not previously identified in vaccine responses (e.g., SPON2, MATK, CST7), and previously uncharacterized genes (e.g. CORO1C, C8orf83) likely related to influenza vaccine-induced immunity due to their expression patterns.
机译:流感疫苗接种后的PBMC转录组包含有关影响疫苗反应因素的宝贵信息。但是,从这些复杂的数据集中提取有意义的知识通常很困难,并且需要先进的数据挖掘算法。我们调查了数据驱动的加权基因相关网络分析(WGCNA)基因聚类方法的使用,以从2010-2011赛季之前和之后的138名健康老年人(50-74岁)收集的PBMC转录组数据集中鉴定疫苗反应相关基因三价流感疫苗接种。 WGCNA根据观察到的跨受试者基因表达模式将14197个基因数据集分为15个基因簇。八个簇强烈富集了涉及特定免疫细胞类型和过程的基因,包括B细胞,T细胞,单核细胞,血小板,NK细胞,细胞毒性T细胞和抗病毒信号传导。对基因簇成员的检查确定了对季节性流感疫苗接种的细胞和体液反应以及先前存在的细胞免疫的特征。这项研究的结果说明了这种公开可用的分析方法的实用性,并突出显示了以前与流感疫苗反应相关的基因(例如CAMK4,CD19),具有疫苗反应中以前未鉴定的功能的基因(例如SPON2,MATK,CST7),以及以前未表征的基因(例如CORO1C,C8orf83)由于其表达方式而与流感疫苗诱导的免疫力有关。

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