Microenvironments in Tuberculous Granulomas Are Delineated by Distinct Populations of Macrophage Subsets and Expression of Nitric Oxide Synthase and Arginase Isoforms

Mattila, Joshua T.; Ojo, Olabisi; Kepka‐Lenhart, Diane; Marino, Simeone; Kim, Jin Hee; Eum, Seok Yong; Via, Laura E.; Barry, Clifton E.; Klein, Edwin; Kirschner, Denise E.; Morris, Sidney M.; Lin, Philana Ling; Flynn, Jo Anne L.

doi:10.4049/jimmunol.1300113

Cited by 296 publications

(419 citation statements)

References 68 publications

(86 reference statements)

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“…The NHP tissue samples were derived from BCG (Bacillus CalmetteGuérin) vaccinated and unvaccinated Mtb-infected rhesus macaques, exhibiting different degrees of lung pathology that was in general inversely correlated with time to end point (survival; Supplementary information, Figure S5A). Immunohistochemical analyses revealed that macrophage infiltration (CD68 + ) increased according to lung pathology severity ( Figure 4A, Supplementary information, Figure S5B); this pattern was also accompanied by increased CD163 expression in tuberculous granulomas in NHPs ( Figure 4A, Supplementary information, Figure S5B) [42]. Concomitantly, we observed an elevated expression of CD16 and MerTK in NHP tuberculous granulomas ( Figure 4A, Supplementary information, Figure S5B).…”

Section: The Abundance Of the Cd16 + Cd163 + Mertk + Pstat3 + Cell Pomentioning

confidence: 61%

“…Considering that the CD16 + population expansion displays an M2-like phenotype in the pleural cavity from TB patients, and that TB pleural effusion activates STAT3 phosphorylation in monocytes from healthy donors and stimulates their protease-dependent migration, we infer that the environmental signals within Mtb infection sites perpetuate the CD16 + CD163 + MerTK + pSTAT3 + activation program and possibly also serve as chemoattractant. At the tissue level, although there are key reports integrating the concept of macrophage activation within tuberculous granulomas [41,42], to our knowledge this is the first study to identify the CD16 + CD163 + MerTK + macrophage activation program along with the co-localization of activated STAT3. Beyond the detection of CD163, we now provide a novel marker signature composed of CD16, MerTK and activated STAT3, which could be helpful to identify the anti-inflammatory and immunomodulatory macrophage program in the progression of TB disease.…”

Section: Discussionmentioning

confidence: 98%

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Tuberculosis is associated with expansion of a motile, permissive and immunomodulatory CD16+ monocyte population via the IL-10/STAT3 axis

et al. 2015

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The human CD14 + monocyte compartment is composed by two subsets based on CD16 expression. We previously reported that this compartment is perturbed in tuberculosis (TB) patients, as reflected by the expansion of CD16 + monocytes along with disease severity. Whether this unbalance is beneficial or detrimental to host defense remains to be elucidated. Here in the context of active TB, we demonstrate that human monocytes are predisposed to differentiate towards an anti-inflammatory (M2-like) macrophage activation program characterized by the CD16 + CD163 + MerTK + pSTAT3 + phenotype and functional properties such as enhanced protease-dependent motility, pathogen permissivity and immunomodulation. This process is dependent on STAT3 activation, and loss-of-function experiments point towards a detrimental role in host defense against TB. Importantly, we provide a critical correlation between the abundance of the CD16 + CD163 + MerTK + pSTAT3 + cells and the progression of the disease either at the local level in a non-human primate tuberculous granuloma context, or at the systemic level through the detection of the soluble form of CD163 in human sera. Collectively, this study argues for the pathogenic role of the CD16 + C-D163 + MerTK + pSTAT3 + monocyte-to-macrophage differentiation program and its potential as a target for TB therapy, and promotes the detection of circulating CD163 as a potential biomarker for disease progression and monitoring of treatment efficacy.

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Section: The Abundance Of the Cd16 + Cd163 + Mertk + Pstat3 + Cell Pomentioning

confidence: 61%

Section: Discussionmentioning

confidence: 98%

Tuberculosis is associated with expansion of a motile, permissive and immunomodulatory CD16+ monocyte population via the IL-10/STAT3 axis

et al. 2015

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“…The predominance of either enzyme spatially influences macrophage activation in different granuloma environments (8,(10)(11)(12)(13). In the presence of oxygen, NOS2 metabolizes L-arginine into L-citrulline and nitric oxide (NO), which is associated with killing of intracellular pathogens (10,(13)(14)(15).…”

mentioning

confidence: 99%

Macrophage arginase-1 controls bacterial growth and pathology in hypoxic tuberculosis granulomas

Duque-Correa¹,

Kühl

Rodríguez

et al. 2014

Proc. Natl. Acad. Sci. U.S.A.

107

109

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Lung granulomas develop upon Mycobacterium tuberculosis (Mtb) infection as a hallmark of human tuberculosis (TB). They are structured aggregates consisting mainly of Mtb-infected and -uninfected macrophages and Mtb-specific T cells. The production of NO by granuloma macrophages expressing nitric oxide synthase-2 (NOS2) via L-arginine and oxygen is a key protective mechanism against mycobacteria. Despite this protection, TB granulomas are often hypoxic, and bacterial killing via NOS2 in these conditions is likely suboptimal. Arginase-1 (Arg1) also metabolizes L-arginine but does not require oxygen as a substrate and has been shown to regulate NOS2 via substrate competition. However, in other infectious diseases in which granulomas occur, such as leishmaniasis and schistosomiasis, Arg1 plays additional roles such as T-cell regulation and tissue repair that are independent of NOS2 suppression. To address whether Arg1 could perform similar functions in hypoxic regions of TB granulomas, we used a TB murine granuloma model in which NOS2 is absent. Abrogation of Arg1 expression in macrophages in this setting resulted in exacerbated lung granuloma pathology and bacterial burden. Arg1 expression in hypoxic granuloma regions correlated with decreased T-cell proliferation, suggesting that Arg1 regulation of T-cell immunity is involved in disease control. Our data argue that Arg1 plays a central role in the control of TB when NOS2 is rendered ineffective by hypoxia.

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“…The high-output pathway of RNS production by host inducible nitric oxide synthase (iNOS) contributes to control of diverse infections (1,2), including tuberculosis (TB) (3,4), via impacts on both the pathogen and the host (5). Macrophages in the lungs of humans (6,7) and macaques (8) with TB express functional iNOS. Correlative evidence suggests that the action of iNOS may contribute to human control of TB (1,3,9,10).…”

mentioning

confidence: 99%

Nitrite produced byMycobacterium tuberculosisin human macrophages in physiologic oxygen impacts bacterial ATP consumption and gene expression

Cunningham‐Bussel¹,

Zhang

Nathan³

2013

Proc. Natl. Acad. Sci. U.S.A.

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In high enough concentrations, such as produced by inducible nitric oxide synthase (iNOS), reactive nitrogen species (RNS) can kill Mycobacterium tuberculosis (Mtb). Lesional macrophages in macaques and humans with tuberculosis express iNOS, and mice need iNOS to avoid succumbing rapidly to tuberculosis. However, Mtb's own ability to produce RNS is rarely considered, perhaps because nitrate reduction to nitrite is only prominent in axenic Mtb cultures at oxygen tensions ≤1%. Here we found that cultures of Mtbinfected human macrophages cultured at physiologic oxygen tensions produced copious nitrite. Surprisingly, the nitrite arose from the Mtb, not the macrophages. Mtb responded to nitrite by ceasing growth; elevating levels of ATP through reduced consumption; and altering the expression of 120 genes associated with adaptation to acid, hypoxia, nitric oxide, oxidative stress, and iron deprivation. The transcriptomic effect of endogenous nitrite was distinct from that of nitric oxide. Thus, whether or not Mtb is hypoxic, the host expresses iNOS, or hypoxia impairs the action of iNOS, Mtb in vivo is likely to encounter RNS by producing nitrite. Endogenous nitrite may slow Mtb's growth and prepare it to resist host stresses while the pathogen waits for immunopathology to promote its transmission.

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Microenvironments in Tuberculous Granulomas Are Delineated by Distinct Populations of Macrophage Subsets and Expression of Nitric Oxide Synthase and Arginase Isoforms

Cited by 296 publications

References 68 publications

Tuberculosis is associated with expansion of a motile, permissive and immunomodulatory CD16+ monocyte population via the IL-10/STAT3 axis

Tuberculosis is associated with expansion of a motile, permissive and immunomodulatory CD16+ monocyte population via the IL-10/STAT3 axis

Macrophage arginase-1 controls bacterial growth and pathology in hypoxic tuberculosis granulomas

Nitrite produced byMycobacterium tuberculosisin human macrophages in physiologic oxygen impacts bacterial ATP consumption and gene expression

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