Macrophage Polarization Drives Granuloma Outcome during Mycobacterium tuberculosis Infection

Marino, Simeone; Cilfone, Nicholas A.; Mattila, Joshua T.; Linderman, Jennifer J.; Flynn, JoAnne L.; Kirschner, Denise E.

doi:10.1128/iai.02494-14

Cited by 154 publications

(162 citation statements)

References 116 publications

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“…IL-10 is an antiinflammatory cytokine that inhibits formation of mature granulomas [37]. A T H 1 to T H 2 shift has long been considered characteristic of HIV-associated immune dysregulation [38], tending to impair granuloma formation [10][11][12]. Further, increased ARG1 expression limits Tcell proliferation, independent of its effect on NO [10].…”

Section: Discussionmentioning

confidence: 99%

“…Among persons with HIV infection, granuloma formation is impaired. Unlike immunocompetent persons, in whom granulomas display a finely organized architecture with spatially modulated gradients of T-cell and macrophage phenotypes [10][11][12], patients with tuberculosis with advanced HIV infection develop disorganized granulomas that are poorly contained collections of polymorphonuclear cells and eosinophils with a paucity of mononuclear, epithelioid, or giant cells [13][14][15][16][17]. Poorly contained lesions in animal tissues are not hypoxic, and this may also be the case in HIV-infected patients with tuberculosis [8,9,18,19].…”

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confidence: 99%

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Adaptation of Mycobacterium tuberculosis to Impaired Host Immunity in HIV-Infected Patients

Walter

Jong

Garcia

et al. 2016

The Journal of Infectious Diseases

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Background. It is unknown whether immunosuppression influences the physiologic state of Mycobacterium tuberculosis in vivo. We evaluated the impact of host immunity by comparing M. tuberculosis and human gene transcription in sputum between human immunodeficiency virus (HIV)-infected and uninfected patients with tuberculosis.Methods. We collected sputum specimens before treatment from Gambians and Ugandans with pulmonary tuberculosis, revealed by positive results of acid-fast bacillus smears. We quantified expression of 2179 M. tuberculosis genes and 234 human immune genes via quantitative reverse transcription-polymerase chain reaction. We summarized genes from key functional categories with significantly increased or decreased expression.Results. A total of 24 of 65 patients with tuberculosis were HIV infected. M. tuberculosis DosR regulon genes were less highly expressed among HIV-infected patients with tuberculosis than among HIV-uninfected patients with tuberculosis (Gambia, P < .0001; Uganda, P = .037). In profiling of human genes from the same sputa, HIV-infected patients had 3.4-fold lower expression of IFNG (P = .005), 4.9-fold higher expression of ARG1 (P = .0006), and 3.4-fold higher expression of IL10 (P = .0002) than in HIVuninfected patients with tuberculosis.Conclusions. M. tuberculosis in HIV-infected patients had lower expression of the DosR regulon, a critical metabolic and immunomodulatory switch induced by NO, carbon monoxide, and hypoxia. Our human data suggest that decreased DosR expression may result from alternative pathway activation of macrophages, with consequent decreased NO expression and/or by poor granuloma formation with consequent decreased hypoxic stress.

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Section: Discussionmentioning

confidence: 99%

mentioning

confidence: 99%

Adaptation of Mycobacterium tuberculosis to Impaired Host Immunity in HIV-Infected Patients

Walter

Jong

Garcia

et al. 2016

The Journal of Infectious Diseases

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“…ESAT-6, a secreted virulence factor not expressed by the attenuated vaccine strain, M. bovis BCG, up-regulated MMP-10 secretion, implicating this pathway in mycobacterial pathology. Furthermore, increased MMP-10 expression has been shown to drive macrophage polarization toward an M2-like phenotype (20), an alternatively activated form of macrophage that is present within TB granulomas and associated with Mtb persistence (38).…”

Section: Discussionmentioning

confidence: 99%

Early Secretory Antigenic Target-6 Drives Matrix Metalloproteinase-10 Gene Expression and Secretion in Tuberculosis

Brilha

Sathyamoorthy

Stuttaford

et al. 2017

Am J Respir Cell Mol Biol

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Tuberculosis (TB) causes disease worldwide, and multidrug resistance is an increasing problem. Matrix metalloproteinases (MMPs), particularly the collagenase MMP-1, cause lung extracellular matrix destruction, which drives disease transmission and morbidity. The role in such tissue damage of the stromelysin MMP-10, a key activator of the collagenase MMP-1, was investigated in direct Mycobacterium tuberculosis (Mtb)-infected macrophages and in conditioned medium from Mtb-infected monocyte-stimulated cells. Mtb infection increased MMP-10 secretion from primary human macrophages 29-fold, whereas Mtb-infected monocytes increased secretion by 4.5-fold from pulmonary epithelial cells and 10.5-fold from fibroblasts. Inhibition of MMP-10 activity decreased collagen breakdown. In two independent cohorts of patients with TB from different continents, MMP-10 was increased in both induced sputum and bronchoalveolar lavage fluid compared with control subjects and patients with other respiratory diseases (both P , 0.05). Mtb drove 3.5-fold greater MMP-10 secretion from human macrophages than the vaccine strain bacillus Calmette-Guerin (P , 0.001), whereas both mycobacteria up-regulated TNF-a secretion equally. Using overlapping, short, linear peptides covering the sequence of early secretory antigenic target-6, a virulence factor secreted by Mtb, but not bacillus Calmette-Guerin, we found that stimulation of human macrophages with a single specific 15-amino acid peptide sequence drove threefold greater MMP-10 secretion than any other peptide (P , 0.001). Mtb-driven MMP-10 secretion was inhibited in a dose-dependent manner by p38 and extracellular signal-related kinase mitogen-activated protein kinase blockade (P , 0.001 and P , 0.01 respectively), but it was not affected by inhibition of NF-kB. In summary, Mtb activates inflammatory and stromal cells to secrete MMP-10, and this is partly driven by the virulence factor early secretory antigenic target-6, implicating it in TB-associated tissue destruction.

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“…At the molecular level, the model accounts for secretion, diffusion, binding, and degradation of cytokines and chemokines. The model has been extensively calibrated to NHP data and successfully predicts granuloma outcomes for tumor necrosis factor alpha (TNF-␣), interleukin-10 (IL-10), and IFN-␥ knockouts (34)(35)(36)(37)(38)(39)(40)(41)61).…”

Section: Methodsmentioning

confidence: 99%

Multiscale Model of Mycobacterium tuberculosis Infection Maps Metabolite and Gene Perturbations to Granuloma Sterilization Predictions

et al. 2016

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cGranulomas are a hallmark of tuberculosis. Inside granulomas, the pathogen Mycobacterium tuberculosis may enter a metabolically inactive state that is less susceptible to antibiotics. Understanding M. tuberculosis metabolism within granulomas could contribute to reducing the lengthy treatment required for tuberculosis and provide additional targets for new drugs. Two key adaptations of M. tuberculosis are a nonreplicating phenotype and accumulation of lipid inclusions in response to hypoxic conditions. To explore how these adaptations influence granuloma-scale outcomes in vivo, we present a multiscale in silico model of granuloma formation in tuberculosis. The model comprises host immunity, M. tuberculosis metabolism, M. tuberculosis growth adaptation to hypoxia, and nutrient diffusion. We calibrated our model to in vivo data from nonhuman primates and rabbits and apply the model to predict M. tuberculosis population dynamics and heterogeneity within granulomas. We found that bacterial populations are highly dynamic throughout infection in response to changing oxygen levels and host immunity pressures. Our results indicate that a nonreplicating phenotype, but not lipid inclusion formation, is important for long-term M. tuberculosis survival in granulomas. We used virtual M. tuberculosis knockouts to predict the impact of both metabolic enzyme inhibitors and metabolic pathways exploited to overcome inhibition. Results indicate that knockouts whose growth rates are below ϳ66% of the wild-type growth rate in a culture medium featuring lipid as the only carbon source are unable to sustain infections in granulomas. By mapping metabolite-and gene-scale perturbations to granuloma-scale outcomes and predicting mechanisms of sterilization, our method provides a powerful tool for hypothesis testing and guiding experimental searches for novel antituberculosis interventions.T uberculosis (TB), caused by inhalation of the pathogen Mycobacterium tuberculosis, is a leading cause of death worldwide (1, 2). The main sites of infection during TB are lung granulomas, dense collections of immune cells and bacteria that develop following infection (3). Understanding M. tuberculosis dynamics within granulomas could aid in development of new antibiotic therapies, since M. tuberculosis growth rates, heterogeneity, and dynamics can affect antibiotic efficacy (3-7).Two in vitro-observed adaptations of M. tuberculosis, suspected to be important in the ability of M. tuberculosis to persist in the host lung, are (i) the adoption of a nonreplicating phenotype and (ii) the accumulation of lipid inclusions, aggregates of neutral lipids inside bacteria (8-13). Hypoxia is known to be a trigger for the transition to a nonreplicating phenotype and the formation of lipid inclusions (9,12,14,15).The in vivo role of the nonreplicating phenotype remains controversial. It has been suggested that M. tuberculosis acquires the nonreplicating phenotype in response to stresses present in the host (such as hypoxia) and that this phenotype allows M. tubercul...

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Macrophage Polarization Drives Granuloma Outcome during Mycobacterium tuberculosis Infection

Cited by 154 publications

References 116 publications

Adaptation of Mycobacterium tuberculosis to Impaired Host Immunity in HIV-Infected Patients

Adaptation of Mycobacterium tuberculosis to Impaired Host Immunity in HIV-Infected Patients

Early Secretory Antigenic Target-6 Drives Matrix Metalloproteinase-10 Gene Expression and Secretion in Tuberculosis

Multiscale Model of Mycobacterium tuberculosis Infection Maps Metabolite and Gene Perturbations to Granuloma Sterilization Predictions

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