Meta-analysis of host response networks identifies a common core in tuberculosis

Sambarey, Awanti; Devaprasad, Abhinandan; Baloni, Priyanka; Mishra, Madhulika; Mohan, Abhilash; Tyagi, Priyanka; Singh, Amit; Akshata, J.S.; Mohammad, Razia Sultana; Buggi, Shashidhar; Chandra, Nagasuma

doi:10.1038/s41540-017-0005-4

Cited by 42 publications

(48 citation statements)

References 58 publications

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“…Compared to the individual analyses of each dataset, the meta-analysis provided increased power to detect only a limited number of differentially regulated genes but most critically identified high confidence differentially regulated gene sets, reducing a large number of false positive markers detected in the individual study analyses. This demonstrated a small overlap of potential biomarkers across multiple studies conducted in different geographical locations, and which agrees with another very recently published meta-analysis of TB ( Sambarey et al, 2017 ). In adults with active TB versus LTBI, 374 genes were differentially regulated and in active TB versus uninfected controls, 332 genes were differentially regulated.…”

Section: Discussionsupporting

confidence: 91%

“…Meta-analyses can provide a statistically stringent and powerful approach to integrate and computationally deconvolute large independent datasets and thereby infer with high confidence new and consistently differentially expressed genes and pathways across multiple studies and age groups. Very recently, several studies have conducted a meta-analysis of a subset of publicly available TB transcriptomic studies; however, none of these meta-analyses studies involved a complete and comprehensive range of both adult and childhood TB ( Sambarey et al, 2017 ; Wang et al, 2018 ) Most notably, the primary data in these studies have yet to be used to identify sentinel immune-metabolic pathways and to deconvolute the proportions of different immune cell types during TB and which are critical in understanding more completely the host systemic responses and for accounting the contribution of specific immune cell type pathways to disease pathogenesis.…”

Section: Introductionmentioning

confidence: 99%

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

et al. 2018

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Background: 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).Methods and findings: 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 (IL1RN and ILR2), 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.Conclusion: 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.

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Section: Discussionsupporting

confidence: 91%

Section: Introductionmentioning

confidence: 99%

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

et al. 2018

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“…This network is termed as human protein–protein interaction network (hPPiN) (Sambarey et al, in press). Briefly, the Search Tool for The Retrieval of Interacting Genes/Proteins (STRING) version 10 (Szklarczyk et al, 2014) was mined to extract all human interactions with a combined score > 900, and the functional nature of these interactions was identified from the protein actions file.…”

Section: Methodsmentioning

confidence: 99%

Unbiased Identification of Blood-based Biomarkers for Pulmonary Tuberculosis by Modeling and Mining Molecular Interaction Networks

et al. 2017

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Efficient diagnosis of tuberculosis (TB) is met with multiple challenges, calling for a shift of focus from pathogen-centric diagnostics towards identification of host-based multi-marker signatures. Transcriptomics offer a list of differentially expressed genes, but cannot by itself identify the most influential contributors to the disease phenotype. Here, we describe a computational pipeline that adopts an unbiased approach to identify a biomarker signature. Data from RNA sequencing from whole blood samples of TB patients were integrated with a curated genome-wide molecular interaction network, from which we obtain a comprehensive perspective of variations that occur in the host due to TB. We then implement a sensitive network mining method to shortlist gene candidates that are most central to the disease alterations. We then apply a series of filters that include applicability to multiple publicly available datasets as well as additional validation on independent patient samples, and identify a signature comprising 10 genes — FCGR1A, HK3, RAB13, RBBP8, IFI44L, TIMM10, BCL6, SMARCD3, CYP4F3 and SLPI, that can discriminate between TB and healthy controls as well as distinguish TB from latent tuberculosis and HIV in most cases. The signature has the potential to serve as a diagnostic marker of TB.

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“…The PLSCR1 gene, located 565 kb away from rs9814705, encodes the transmembrane protein phospholipid scramblase 1, which has been shown to be overexpressed after stimulation with type I interferons, and to play a crucial role in apoptosis 36,37 . This gene has also been identified as a core gene in the host response to tuberculosis in a meta-analysis of transcriptomic data 38 . Thus, PLSCR1 may be an interesting candidate gene for involvement in the development of Buruli ulcer.…”

Section: Discussionmentioning

confidence: 99%

Genome-wide association study of Buruli ulcer in rural Benin highlights role of two LncRNAs and the autophagy pathway

et al. 2020

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Buruli ulcer, caused by Mycobacterium ulcerans and characterized by devastating necrotizing skin lesions, is the third mycobacterial disease worldwide. The role of host genetics in susceptibility to Buruli ulcer has long been suggested. We conduct the first genome-wide association study of Buruli ulcer on a sample of 1524 well characterized patients and controls from rural Benin. Two-stage analyses identify two variants located within LncRNA genes: rs9814705 in ENSG00000240095.1 (P = 2.85 × 10 −7 ; odds ratio = 1.80 [1.43-2.27]), and rs76647377 in LINC01622 (P = 9.85 × 10 −8 ; hazard ratio = 0.41 [0.28-0.60]). Furthermore, we replicate the protective effect of allele G of a missense variant located in ATG16L1, previously shown to decrease bacterial autophagy (rs2241880, P = 0.003; odds ratio = 0.31 [0.14-0.68]). Our results suggest LncRNAs and the autophagy pathway as critical factors in the development of Buruli ulcer.

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Meta-analysis of host response networks identifies a common core in tuberculosis

Cited by 42 publications

References 58 publications

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

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

Unbiased Identification of Blood-based Biomarkers for Pulmonary Tuberculosis by Modeling and Mining Molecular Interaction Networks

Genome-wide association study of Buruli ulcer in rural Benin highlights role of two LncRNAs and the autophagy pathway

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