Transcriptional landscape of Mycobacterium tuberculosis infection in macrophages

Roy, Sugata; Schmeier, Sebastian; Kaczkowski, Bogumił; Arner, Peter; Alam, Tanvir; Ozturk, Mumin; Tamgue, Ousman; Parihar, Suraj P.; Kawaji, Hideya; Itoh, Masayoshi; Lassmann, Timo; Carninci, Piero; Hayashizaki, Yoshihide; Forrest, Alistair R.R.; Guler, Reto; Bajic, Vladimir B.; Brombacher, Frank; Suzuki, Harukazu

doi:10.1038/s41598-018-24509-6

Cited by 83 publications

(111 citation statements)

References 43 publications

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“…Previous reports have shown that EGR1 regulates ATF3 expression in murine αT3-1 cells (Mayer, Dexheimer, Nishida, Kitajima, & Thiel, 2008). Both we and others have observed through global transcriptome profiling that challenge of macrophages with M. tuberculosis leads to an early upregulation of EGR1 (Kumar et al, 2015;Roy et al, 2018). In this study, we validated the early upregulation of EGR1 transcript in infected RAW264.7 ( Figure 2a) and BMDMs ( Figure 2b).…”

Section: Transcriptional Regulation Of Atf3 Is Dependent Upon Egr1 supporting

confidence: 74%

“…It is ubiquitously expressed and is induced upon challenge of a variety of cell types by bacteria (de Klerk, Saroj, Wassing, Maudsdotter, & Jonsson, 2017). Both we and others have observed through global transcriptome profiling that challenge of macrophages with M. tuberculosis leads to an early upregulation of EGR1 (Kumar et al, 2015;Roy et al, 2018). Both we and others have observed through global transcriptome profiling that challenge of macrophages with M. tuberculosis leads to an early upregulation of EGR1 (Kumar et al, 2015;Roy et al, 2018).…”

Section: Transcriptional Regulation Of Atf3 Is Dependent Upon Egr1 mentioning

confidence: 70%

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Activating transcription factor 3 modulates the macrophage immune response toMycobacterium tuberculosisinfection via reciprocal regulation of inflammatory genes and lipid body formation

Kumar

Majumder

Mal

et al. 2019

Cellular Microbiology

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Infection of macrophages by Mycobacterium tuberculosis elicits an immune response that clears the bacterium. However, the bacterium is able to subvert the innate immune response. Differential expression of transcription factors (TFs) is central to the dynamic balance of this interaction. Among other functions, TFs regulate the production of antibacterial agents such as nitric oxide, pro-inflammatory cytokines and neutral lipids which are stored in lipid bodies (LBs) and favour bacterial survival. Here, we demonstrate that the TF activating transcription factor 3 (ATF3) is upregulated early during infection of macrophages or mice. Depletion of ATF3 enhances mycobacterial survival in macrophages suggesting its host-protective role. ATF3 interacts with chromatin remodelling protein brahma-related gene 1 and both associate with the promoters of interleukin-12p40, interleukin-6 and nitric oxide synthase 2, to activate expression of these genes. Strikingly, ATF3 downregulates LB formation by associating at the promoters of positive regulators of LB formation such as cholesterol 25 hydroxylase and the microRNA-33 locus. ATF3 represses the association of the activating mark, acetyl histone H4 lysine 8 at the promoter of cholesterol 25 hydroxylase. Our study suggests opposing roles of ATF3 in regulation of distinct sets of macrophage genes during infection, converging on a host-protective immune response.

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Section: Transcriptional Regulation Of Atf3 Is Dependent Upon Egr1 supporting

confidence: 74%

Section: Transcriptional Regulation Of Atf3 Is Dependent Upon Egr1 mentioning

confidence: 70%

Activating transcription factor 3 modulates the macrophage immune response toMycobacterium tuberculosisinfection via reciprocal regulation of inflammatory genes and lipid body formation

Kumar

Majumder

Mal

et al. 2019

Cellular Microbiology

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“…It is thought that Th2 cytokines such as IL-13 can cause inappropriate activation of macrophages and thus, undermine the Th1 response suitable for an intracellular pathogen like Mtb. 21 We also found increased levels of IL-17A, IP-10 and MIP1β in converters compared with nonconverters. IL-17A is associated with Th17 responses with a previous study from our laboratory showing contrasting findings (ie, increased IL-17A in TBR).…”

Section: Discussionsupporting

confidence: 53%

Analysis of cellular and soluble profiles in QuantiFERON nonconverters, converters, and reverters in the Gambia

Medawar

Tukiman

Mbayo

et al. 2019

Immunity Inflam & Disease

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Background Tuberculosis (TB) is the leading cause of death from a single infectious agent worldwide. The immune system is capable of clearing the pathogen before establishment of latent infection but the mechanisms for this are not yet understood. Methods This study analysed highly exposed household contacts (HHC) of TB index cases who were categorised according to QuantiFERON (QFT) results at recruitment and 6 months. Seventeen (17) QFT nonconverters, 14 QFT converters, 18 QFT reverters and 18 latent TB infection (LTBI) were analysed. Supernatants generated following QFT stimulation at both time‐points were analysed using a 64‐plex cytokine array. Flow cytometry was performed on QFT converters and nonconverters at baseline only. Results Interleukin‐2 (IL‐2), IL‐5, IL‐13, APRIL, IL‐17A, IP‐10, MIP‐1ß, sIL‐6rb, OPN, and sTNFR2 were all significantly higher in the QFT converters compared with nonconverters at baseline. Levels of interferon‐α2 (IFN‐α2) and IL‐2 were significantly lower in QFT reverters compared with nonconverters at baseline. Analysis of Ag‐specific IL‐2 levels resulted in an area under the curve (AUC) of 0.93 (95% confidence interval [CI], 0.84‐1.00) for QFT converters compared to nonconverters and an AUC of 0.80 (0.65‐0.95) for QFT reverters compared with LTBI. Purified protein derivative (PPD)‐specific CD4 + CD26 + IFN‐γ + cells were significantly increased (P = .0007) in QFT nonconverters compared with QFT converters at baseline. Conclusions Our results provide insight into the underlying mechanisms of resistance to sustained Mycobacterium tuberculosis infection.

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“…In the later stages and chronic disease, the infection is associated with responses mediated by M2 macrophages, whose weak microbicidal activity and ability to eliminate bacteria are linked to the occurrence of the lesions observed during disease evolution. [265][266][267][268][269] In leprosy, macrophages are the primary cells that exert microbicidal activity. Thus, the role of macrophages in the response to M. leprae has been widely described and is correlated with the expression of certain cytokines that are classical representatives of the cellular immune response, such as TNF-α and IFN-γ.…”

Section: Autophagymentioning

confidence: 99%

<p>Functional aspects, phenotypic heterogeneity, and tissue immune response of macrophages in infectious diseases</p>

Sousa¹,

Vasconcelos²,

Quaresma³

2019

IDR

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Macrophages are a functionally heterogeneous group of cells with specialized functions depending not only on their subgroup but also on the function of the organ or tissue in which the cells are located. The concept of macrophage phenotypic heterogeneity has been investigated since the 1980s, and more recent studies have identified a diverse spectrum of phenotypic subpopulations. Several types of macrophages play a central role in the response to infectious agents and, along with other components of the immune system, determine the clinical outcome of major infectious diseases. Here, we review the functions of various macrophage phenotypic subpopulations, the concept of macrophage polarization, and the influence of these cells on the evolution of infections. In addition, we emphasize their role in the immune response in vivo and in situ, as well as the molecular effectors and signaling mechanisms used by these cells. Furthermore, we highlight the mechanisms of immune evasion triggered by infectious agents to counter the actions of macrophages and their consequences. Our aim here is to provide an overview of the role of macrophages in the pathogenesis of critical transmissible diseases and discuss how elucidation of this relationship could enhance our understanding of the host–pathogen association in organ-specific immune responses.

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Transcriptional landscape of Mycobacterium tuberculosis infection in macrophages

Cited by 83 publications

References 43 publications

Activating transcription factor 3 modulates the macrophage immune response toMycobacterium tuberculosisinfection via reciprocal regulation of inflammatory genes and lipid body formation

Activating transcription factor 3 modulates the macrophage immune response toMycobacterium tuberculosisinfection via reciprocal regulation of inflammatory genes and lipid body formation

Analysis of cellular and soluble profiles in QuantiFERON nonconverters, converters, and reverters in the Gambia

<p>Functional aspects, phenotypic heterogeneity, and tissue immune response of macrophages in infectious diseases</p>

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