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荟萃分析:鉴定儿童和成人对急性和潜伏性结核病全身宿主反应的高度稳健和差异性免疫代谢特征

Meta-Analysis Identification of Highly Robust and Differential Immune-Metabolic Signatures of Systemic Host Response to Acute and Latent Tuberculosis in Children and Adults.

作者信息

Bah Saikou Y, Forster Thorsten, Dickinson Paul, Kampmann Beate, Ghazal Peter

机构信息

Division of Pathway Medicine and Edinburgh Infectious Diseases, University of Edinburgh Medical School, Edinburgh, United Kingdom.

West African Centre for Cellular Biology of Infectious Pathogens, University of Ghana, Accra, Ghana.

出版信息

Front Genet. 2018 Oct 4;9:457. doi: 10.3389/fgene.2018.00457. eCollection 2018.

Abstract

Whole blood expression profiling is a mainstay for delineating differential diagnostic signatures of infection yet is subject to high variability that reduces power and complicates clinical usefulness. To date, confirmatory high confidence expression profiling signatures for clinical use remain uncertain. Here we have sought to evaluate the reproducibility and confirmatory nature of differential expression signatures, comprising molecular and cellular pathways, across multiple international clinical observational studies investigating children and adult whole blood transcriptome responses to tuberculosis (TB). A systematic search and quality control assessment of gene expression repositories for human TB using whole blood resulted in 11 datasets with a total of 1073 patients from Africa, Europe, and South America. A non-parametric estimation of percentage of false prediction was used for meta-analysis of high confidence differential expression analysis. Deconvolution analysis was applied to infer changes in immune cell proportions and enrichment tests applied using pathway database resources. Meta-analysis identified high confidence differentially expressed genes, comprising 372 in adult active-TB versus latent-TB (LTBI), 332 in adult active-TB versus controls (CON), five in LTBI versus CON, and 415 in childhood active-TB versus LTBI. Notably, these confirmatory markers have low representation in published signatures for diagnosing TB. Pathway biology analysis of high confidence gene sets revealed dominant metabolic and innate-immune pathway signatures while suppressed signatures were enriched with adaptive signaling pathways and reduced proportions of T and B cells. Childhood TB showed uniquely strong inflammasome antagonist signature ( and ), while adult TB patients exhibit a significant preponderance type I and type II IFN markers. Key limitations of the study include the paucity of data on potential confounders. Meta-analysis identified high confidence confirmatory immune-metabolic and cellular expression signatures across studies regardless of the population resource setting, HIV status and circulating endemic pathogens. Notably, previously identified diagnostic signature markers for TB show limited concordance with the confirmatory meta-analysis. Overall, our results support the use of the confirmatory expression signatures for guiding optimized diagnostic, prognostic, and therapeutic monitoring modalities in TB.

摘要

全血表达谱分析是描绘感染鉴别诊断特征的主要方法,但存在高度变异性,这降低了效能并使临床应用复杂化。迄今为止,用于临床的高可信度确认性表达谱特征仍不明确。在此,我们试图评估差异表达特征(包括分子和细胞途径)在多项国际临床观察性研究中的可重复性和确认性质,这些研究调查了儿童和成人全血转录组对结核病(TB)的反应。使用全血对人类结核病基因表达库进行系统搜索和质量控制评估,得到了11个数据集,共1073名来自非洲、欧洲和南美洲的患者。采用非参数错误预测百分比估计法对高可信度差异表达分析进行荟萃分析。应用反卷积分析来推断免疫细胞比例的变化,并使用通路数据库资源进行富集测试。荟萃分析确定了高可信度的差异表达基因,其中成人活动性结核病与潜伏性结核病(LTBI)相比有372个,成人活动性结核病与对照(CON)相比有332个,LTBI与CON相比有5个,儿童活动性结核病与LTBI相比有415个。值得注意的是,这些确认性标志物在已发表的结核病诊断特征中代表性较低。对高可信度基因集的通路生物学分析揭示了主要的代谢和固有免疫通路特征,而受抑制的特征则富集了适应性信号通路以及T细胞和B细胞比例的降低。儿童结核病表现出独特的强烈炎性小体拮抗剂特征(和),而成人结核病患者则表现出显著占优势的I型和II型干扰素标志物。该研究的主要局限性包括潜在混杂因素的数据匮乏。荟萃分析确定了跨研究的高可信度确认性免疫代谢和细胞表达特征,无论人群资源设置如何、HIV状态以及循环流行病原体情况如何。值得注意的是,先前确定的结核病诊断特征标志物与确认性荟萃分析的一致性有限。总体而言,我们的结果支持使用确认性表达特征来指导结核病的优化诊断、预后和治疗监测模式。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/95b1/6180280/6a500ec63238/fgene-09-00457-g001.jpg

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