CD14 regulates the dendritic cell life cycle after LPS exposure through NFAT activation

Zanoni, Ivan; Ostuni, Renato; Capuano, Giusy; Collini, Maddalena; Caccia, Michele; Rocchetti, Marcella; Mingozzi, Francesca; Foti, Maria; Chirico, Giuseppe; Costa, Barbara; Zaza, Antonio; Ricciardi‐Castagnoli, Paola; Granucci, Francesca

doi:10.1038/nature08118

Cited by 282 publications

(333 citation statements)

References 33 publications

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“…Here, we show that TLR4‐specific ultrapure (up)LPS‐primed phenotypically activated BMDC, rather than worsening the severity of EAU, significantly prevent the development of EAU. We show that upLPS‐primed BMDC are endotoxin homotolerant (ET‐BMDC) and further show that they are heterotolerant to M. tuberculosis protein extract in that they are (i) susceptible to apoptosis45, 46, 47 (confirmed here) through a CD14/nuclear factor of activated T cells (NFATc)‐associated mechanism, and (ii) fail to secrete IL‐1 β on exposure to M. tuberculosis extract. As M. tuberculosis mediated C‐type lectin receptor signalling via the Syk/CARD‐9 complex,48 a major route for inflammasome activation, has been shown to be an essential mediator of IRBP‐CFA‐induced EAU,48, 49 we propose that inhibition of IL‐1 β secretion is one mechanism whereby heterotolerant LPS‐primed BMDC promote immunological tolerance.…”

Section: Introductionsupporting

confidence: 55%

“…Zanoni et al 30, 47, 77. have shown that LPS‐primed BMDC are programmed for apoptosis, unlike LPS‐primed macrophages which, although refractory to a second challenge of LPS, survive in culture for prolonged periods.…”

Section: Discussionmentioning

confidence: 99%

“…3). 47 Apoptotic cells are known to promote immune tolerance when administered in vivo . In particular, the clearance of apoptotic cells has been identified as an event that is directly responsible for tolerance induction.…”

Section: Discussionmentioning

confidence: 99%

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Lipopolysaccharide‐primed heterotolerant dendritic cells suppress experimental autoimmune uveoretinitis by multiple mechanisms

et al. 2016

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SummaryExposure of bone‐marrow‐derived dendritic cells (BMDC) to high‐dose ultrapure lipopolysaccharide for 24 hr (LPS‐primed BMDC) enhances their potency in preventing inter‐photoreceptor retinoid binding protein: complete Freund's adjuvant‐induced experimental autoimmune uveoretinitis (EAU). LPS‐primed BMDC are refractory to further exposure to LPS (= endotoxin tolerance), evidenced here by decreased phosphorylation of TANK‐binding kinase 1, interferon regulatory factor 3 (IRF3), c‐Jun N‐terminal kinase and p38 mitogen‐activated protein kinase as well as impaired nuclear translocation of nuclear factor κB (NF‐κB) and IRF3, resulting in reduced tumour necrosis factor‐α (TNF‐α), interleukin‐6 (IL‐6), IL‐12 and interferon‐β secretion. LPS‐primed BMDC also show reduced surface expression of Toll‐like receptor‐4 and up‐regulation of CD14, followed by increased apoptosis, mediated via nuclear factor of activated T cells (NFATc)‐2 signalling. LPS‐primed BMDC are not only homotolerant to LPS but are heterotolerant to alternative pathogen‐associated molecular pattern ligands, such as mycobacterial protein extract (Mycobacterium tuberculosis). Specifically, while M. tuberculosis protein extract induces secretion of IL‐1β, TNF‐α and IL‐6 in unprimed BMDC, LPS‐primed BMDC fail to secrete these cytokines in response to M. tuberculosis. We propose that LPS priming of BMDC, by exposure to high doses of LPS for 24 hr, stabilizes their tolerogenicity rather than promoting immunogenicity, and does so by multiple mechanisms, namely (i) generation of tolerogenic apoptotic BMDC through CD14:NFATc signalling; (ii) reduction of NF‐κB and IRF3 signalling and downstream pro‐inflammatory cytokine production; and (iii) blockade of inflammasome activation.

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Section: Introductionsupporting

confidence: 55%

Section: Discussionmentioning

confidence: 99%

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Lipopolysaccharide‐primed heterotolerant dendritic cells suppress experimental autoimmune uveoretinitis by multiple mechanisms

et al. 2016

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“…Macrophages develop from hematopoietic stem cells through common myeloid progenitors in the BM, and repopulate in peripheral tissues [2]. Currently, macrophages can be classified into several different subtypes, based on their reactions to different stimuli [3][4][5]. Macrophages involved in inflammatory responses to bacterial and viral infection are called M1 macrophages.…”

Section: Conflict Ofmentioning

confidence: 99%

“…Regardless of classification controversies about cells of the myelomonocytic lineage, an example of their functional peculiarities is the non-overlapping responsiveness of macrophages and DCs to the prototypical toll-like receptor 4 (TLR4) stimulator lipopolysaccharide (LPS), with features that can only be partially explained by differences in the expression of responder proteins [3]. Adding complexity to the picture is the action of tissue-specific microenvironmental cues, which likely control specialized behaviors and fine-tune cellular identities, in fact representing developmental modifiers operating on differentiated cells [4].…”

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confidence: 99%

Transcriptional control of macrophage diversity and specialization

Ostuni

Natoli

2011

Eur J Immunol

Self Cite

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The key driving force underlying cell identity is represented by the complex and dynamic interplay between cell‐intrinsic, lineage‐restricted developmental pathways on the one hand, and cell‐extrinsic, tissue‐specific microenvironmental signals on the other. In this context, macrophages are a paradigmatic cell population whose functional specialization in vivo reflects the impact of the local microenvironment on the intrinsic differentiation program, leading to a variety of specialized macrophage types in different tissues and conditions; however, how this is translated into a biological outcome is not appreciably understood. The kind of investigations described in this Viewpoint aim to explore the inner determinants of cell identity and functional diversification at a genomic level; mechanisms that permit plastic cell types, like macrophages, to adapt to different environments.

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Modification of pro‐inflammatory signaling by dietary components: The plasma membrane as a target

Ciesielska

Kwiatkowska

2015

BioEssays

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You are what you eat - this well-known phrase properly describes the phenomenon of the effects of diet on acute and chronic inflammation. Several lipids and lipophilic compounds that are delivered with food or are produced in situ in pathological conditions exert immunomodulatory activity due to their interactions with the plasma membrane. This group of compounds includes cholesterol and its oxidized derivatives, fatty acids, α-tocopherol, and polyphenols. Despite their structural heterogeneity, all these compounds ultimately induce changes in plasma membrane architecture and fluidity. By doing this, they modulate the dynamics of plasma membrane receptors, such as TLR4. This receptor is activated by lipopolysaccharide, triggering acute inflammation during bacterial infection, which often leads to sepsis and is linked with diverse chronic inflammatory diseases. In this review, we discuss how the impact on plasma membrane properties contributes to the immunomodulatory activity of dietary compounds, pointing to the therapeutic potential of some of them. Also watch the Video Abstract.

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CD14 regulates the dendritic cell life cycle after LPS exposure through NFAT activation

Cited by 282 publications

References 33 publications

Lipopolysaccharide‐primed heterotolerant dendritic cells suppress experimental autoimmune uveoretinitis by multiple mechanisms

Lipopolysaccharide‐primed heterotolerant dendritic cells suppress experimental autoimmune uveoretinitis by multiple mechanisms

Transcriptional control of macrophage diversity and specialization

Modification of pro‐inflammatory signaling by dietary components: The plasma membrane as a target

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