Innate immune system favors emergency monopoiesis at the expense of DC‐differentiation to control systemic bacterial infection in mice

Pasquevich, Karina A.; Bieber, Kristin; Günter, Manina; Grauer, Matthias; Pötz, Oliver; Schleicher, Ulrike; Biedermann, Tilo; Beer‐Hammer, Sandra; Bühring, Hans‐Jörg; Rammensee, Hans‐Georg; Zender, Lars; Autenrieth, Ingo B.; Lengerke, Claudia; Autenrieth, Stella E.

doi:10.1002/eji.201545530

Cited by 24 publications

(31 citation statements)

References 56 publications

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“…To determine the effects of LPS on cMoPs, bone marrow cells were counted in WT mice after an injection of LPS or PBS. As reported previously in the context of bacterial infection 45 , a significant drop in the number of cMoP precursor cells was observed 24 h after LPS injection (Fig. 3A and B ).…”

Section: Resultssupporting

confidence: 88%

“…To determine whether this decrease in cMoPs resulted from accelerated differentiation into monoblasts and promonocyte (pro-Mo) cells (as suggested by 45 ), we counted these precursors in the bone marrow. Monoblasts were defined as live singlet Lin − CD115 + CD11c − MHCII − Ly6C + Sca-1 + CD11b − cells, and pro-Mo cells were defined as live singlet Lin − CD115 + CD11c − MHCII − Ly6C + Sca-1 + CD11b + cells 45 . We detected a significant increase in the number of monoblasts and pro-Mo cells within the bone marrow after LPS injection when compared to PBS injection (Fig.…”

Section: Resultsmentioning

confidence: 99%

“…As positive and negative effects of type-I IFN on HSPCs are described in the literature 37 , we measured the proliferation and number of LSK bone marrow cells (Lin − Sca-1 + c-kit + ) 45 , 46 . LSK cells were gated as described in Supplementary Figure S4A 45 , and a significant increase of their number and proliferation, evaluated by BrdU incorporation, was observed in a type-I IFN independent manner (see Supplementary Figure S4B ). Then, LPS induced the generation of monocyte precursors 24 h after its injection in a type-I dependent manner.…”

Section: Resultsmentioning

confidence: 99%

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Type I interferons drive inflammasome-independent emergency monocytopoiesis during endotoxemia

Lasseaux

Fourmaux

Chamaillard

et al. 2017

Sci Rep

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Emergency monocytopoiesis is an inflammation-driven hematological process that supplies the periphery with monocytes and subsequently with macrophages and monocyte-derived dendritic cells. Yet, the regulatory mechanisms by which early bone marrow myeloid progenitors commit to monocyte-derived phagocytes during endotoxemia remains elusive. Herein, we show that type I interferons signaling promotes the differentiation of monocyte-derived phagocytes at the level of their progenitors during a mouse model of endotoxemia. In this model, we characterized early changes in the numbers of conventional dendritic cells, monocyte-derived antigen-presenting cells and their respective precursors. While loss of caspase-1/11 failed to impair a shift toward monocytopoiesis, we observed sustained type-I-IFN-dependent monocyte progenitors differentiation in the bone marrow correlated to an accumulation of Mo-APCs in the spleen. Importantly, IFN-alpha and -beta were found to efficiently generate the development of monocyte-derived antigen-presenting cells while having no impact on the precursor activity of conventional dendritic cells. Consistently, the LPS-driven decrease of conventional dendritic cells and their direct precursor occurred independently of type-I-IFN signaling in vivo. Our characterization of early changes in mononuclear phagocytes and their dependency on type I IFN signaling during sepsis opens the way to the development of treatments for limiting the immunosuppressive state associated with sepsis.

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Section: Resultssupporting

confidence: 88%

Section: Resultsmentioning

confidence: 99%

Section: Resultsmentioning

confidence: 99%

See 1 more Smart Citation

Type I interferons drive inflammasome-independent emergency monocytopoiesis during endotoxemia

Lasseaux

Fourmaux

Chamaillard

et al. 2017

Sci Rep

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“…In immunocompromised patients, systemic infection can lead to focal abscesses in the spleen and liver [ 9 ]. Similar clinical manifestations have been found in a murine model of systemic Yersinia infection, with Ye also being detectable in the lymph nodes, bone marrow and lungs at one day post-infection [ 10 - 11 ]. The virulence of Ye is associated with Yersinia adhesin A (YadA), a trimeric autotransporter that mediates cell adhesion.…”

Section: Introductionsupporting

confidence: 65%

New pathogen-specific immunoPET/MR tracer for molecular imaging of a systemic bacterial infection

et al. 2016

Self Cite

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The specific and rapid detection of Enterobacteriaceae, the most frequent cause of gram-negative bacterial infections in humans, remains a major challenge. We developed a non-invasive method to rapidly detect systemic Yersinia enterocolitica infections using immunoPET (antibody-targeted positron emission tomography) with [64Cu]NODAGA-labeled Yersinia-specific polyclonal antibodies targeting the outer membrane protein YadA. In contrast to the tracer [18F]FDG, [64Cu]NODAGA-YadA uptake co-localized in a dose dependent manner with bacterial lesions of Yersinia-infected mice, as detected by magnetic resonance (MR) imaging. This was accompanied by elevated uptake of [64Cu]NODAGA-YadA in infected tissues, in ex vivo biodistribution studies, whereas reduced uptake was observed following blocking with unlabeled anti-YadA antibody. We show, for the first time, a bacteria-specific, antibody-based, in vivo imaging method for the diagnosis of a Gram-negative enterobacterial infection as a proof of concept, which may provide new insights into pathogen-host interactions.

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“…During sepsis, emergency myelopoiesis is triggered in the bone marrow in response to signals from G-CSF released in the blood by the injured endothelium [ 41 , 58 , 59 ]. Hematopoietic stem cells proliferate giving rise to neutrophils that egress from the bone marrow and enter the circulation [ 41 , 60 ].…”

Section: Discussionmentioning

confidence: 99%

Cannabinoid Receptor 2 Modulates Neutrophil Recruitment in a Murine Model of Endotoxemia

Kapellos

Recio

Greaves

et al. 2017

Mediators of Inflammation

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The endocannabinoid system consists of endogenous lipid mediators and cannabinoid receptors (CB) 1 and 2. It has previously been demonstrated that activation of the leukocyte-expressed CB2 has anti-inflammatory effects in vivo. Here, we report its role under baseline conditions and in a model of low-dose endotoxemia by comparing CB2 knockout to littermate control mice. CB2-deficient mice displayed significantly more neutrophils and fewer monocytes in the bone marrow under steady state. In initial validation experiments, administration of 1 mg/kg LPS to male C57BL/6J mice was shown to transiently upregulate systemic proinflammatory mediators (peaked at 2 hours) and mobilise bone marrow neutrophils and monocytes into circulation. In CB2 knockout mice, the level of the metalloproteinase MMP-9 was significantly elevated by 2 hours and we also observed augmented recruitment of neutrophils to the spleen in addition to increased levels of Ccl2, Ccl3, Cxcl10, and Il6. Collectively, our data show that the absence of CB2 receptor increases the levels of innate immune cell populations in the bone marrow under steady state. Furthermore, during an acute systemic inflammatory insult, we observe a highly reproducible and site-specific increase in neutrophil recruitment and proinflammatory chemokine expression in the spleen of CB2 knockout mice.

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Innate immune system favors emergency monopoiesis at the expense of DC‐differentiation to control systemic bacterial infection in mice

Cited by 24 publications

References 56 publications

Type I interferons drive inflammasome-independent emergency monocytopoiesis during endotoxemia

Type I interferons drive inflammasome-independent emergency monocytopoiesis during endotoxemia

New pathogen-specific immunoPET/MR tracer for molecular imaging of a systemic bacterial infection

Cannabinoid Receptor 2 Modulates Neutrophil Recruitment in a Murine Model of Endotoxemia

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