Network dynamics determine the autocrine and paracrine signaling functions of TNF

Caldwell, Andrew B.; Zhang, Cheng; Vargas, Jesse D.; Birnbaum, Harry; Hoffmann, Alexander

doi:10.1101/gad.244749.114

Cited by 84 publications

(127 citation statements)

References 64 publications

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“…Like IFNα, TNFα was predicted to be involved in an autocrine loop in MDM elicited by LPS, since the TNFα receptor is also induced 27. Our data (Supplemental Table S2) confirm and extend evidence of autocrine TNFα signaling as a feed‐forward activator of macrophage gene expression30, 62, 63 and identify the subset of inducible genes dependent upon that stimulus. The lack of impact of anti‐TNFα on LPS‐inducible IDO1 may reflect the magnitude of the response.…”

Section: Discussionsupporting

confidence: 72%

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Effects of anti-inflammatory drugs on the expression of tryptophan-metabolism genes by human macrophages

Regan

Gill

Clohisey

et al. 2018

Journal of Leukocyte Biology

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Several lines of evidence link macrophage activation and inflammation with (monoaminergic) nervous systems in the etiology of depression. IFN treatment is associated with depressive symptoms, whereas anti‐TNFα therapies elicit positive mood. This study describes the actions of 2 monoaminergic antidepressants (escitalopram, nortriptyline) and 3 anti‐inflammatory drugs (indomethacin, prednisolone, and anti‐TNFα antibody) on the response of human monocyte‐derived macrophages (MDMs) from 6 individuals to LPS or IFN‐α. Expression profiling revealed robust changes in the MDM transcriptome (3294 genes at P < 0.001) following LPS challenge, whereas a more limited subset of genes (499) responded to IFNα. Contrary to published reports, administered at nontoxic doses, neither monoaminergic antidepressant significantly modulated the transcriptional response to either inflammatory challenge. Each anti‐inflammatory drug had a distinct impact on the expression of inflammatory cytokines and on the profile of inducible gene expression—notably on the regulation of enzymes involved in metabolism of tryptophan. Inter alia, the effect of anti‐TNFα antibody confirmed a predicted autocrine stimulatory loop in human macrophages. The transcriptional changes were predictive of tryptophan availability and kynurenine synthesis, as analyzed by targeted metabolomic studies on cellular supernatants. We suggest that inflammatory processes in the brain or periphery could impact on depression by altering the availability of tryptophan for serotonin synthesis and/or by increasing production of neurotoxic kynurenine.

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Section: Discussionsupporting

confidence: 72%

“…Alternatively, activation of IDO1 by IFN‐γ requires co‐stimulation by TNFα, which increases the occupancy of IFN‐response elements 64, 65. It may be that LPS provides this second signal independently of TNFα 30, 62, 63…”

Section: Discussionmentioning

confidence: 99%

Effects of anti-inflammatory drugs on the expression of tryptophan-metabolism genes by human macrophages

Regan

Gill

Clohisey

et al. 2018

Journal of Leukocyte Biology

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“…Cytokines like TNF and TGF-β trigger behavioural changes or differentiation of nearby celltypes through paracrine signalling in mammals (Derynck and Akhurst 2007;Caldwell, et al 2014), and the upregulation of these cytokines in my experiments suggests they too could participate in coordinating the sponge cellular response to bacteria. TNF in particular is upregulated in choanocytes compared to the other two cells types, and it is possible that choanocytes release TNF ligands to communicate with other cell-types in the vicinity of choanocyte chambers.…”

Section: Tnf Ligandmentioning

confidence: 86%

“…The MyD88-dependent pathway has an ancient, highly conserved role regulating humoral aspects of immunity through antimicrobial peptide (AMP) production in animals as diverse as Hydra, Drosophila and humans (Tauszig, et al 2000;). TNF signalling, on the other hand, is important for the coordination of cellular immunity through autocrine or paracrine signalling (Caldwell, et al 2014). Indeed, the Drosophila TNF ligand, Eiger, is an important modulator of phagocytic activity, and Eiger-mutant flies show decreased phagocytosis and thus reduced clearance of extracellular pathogens (Schneider, et al 2007).…”

Section: A Queenslandicamentioning

confidence: 99%

Deciphering the genomic toolkit underlying animal-bacteria interactions – insights through the demosponge Amphimedon queenslandica

Yuen¹

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All animals are inhabited by bacteria, and maintaining homeostasis in the multicellular environment of the host involves the complex balancing act of promoting the survival of symbionts while defending against intruders. Sponges (Porifera), in addition to housing diverse bacterial symbiont assemblages, also rely on bacteria filtered from the water column for nutrition. My research uses the genome-enabled demosponge, Amphimedon queenslandica, a member of one of the earliest-diverging animal phyletic lineages, as an experimental platform to investigate the genomic toolkit underpinning animal-bacteria interactions. Using comparative bioinformatics tools, I characterised a surprisingly large and complex repertoire of innate immune receptors from the NLR family of genes encoded in the A. queenslandica genome. I then used a high throughput RNAseq approach to profile the sponge's global transcriptomic response to foreign versus its own native bacteria. Conserved metazoan innate immune pathways were activated in response to both foreign and native bacteria. However, only the native bacteria elicited the expression of a more extensive suite of signalling pathways, involving TGF-β signalling and the transcription factors NF-κB and FoxO. Upregulation of the nutrient sensor AMPK in all treatments along with immune signalling genes, which all regulate FoxO activity, further suggests an interplay between metabolic homeostasis and immunity. Finally, I used microscopy to track the cellular-level processing of the different bacteria by the sponge. Consistent with the observed transcriptional response, the native bacteria were ingested by archaeocytes more rapidly than the foreign bacteria. The slower processing of foreign bacteria also correlated with the expression of numerous Nrf2-associated detoxification genes, indicative of cellular stress, only in response to foreign bacteria.iii Deciphering the genomic tool-kit underlying animal-bacteria interactions

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“…However, once monocytes adhere, they infiltrate into the lesions and differentiate into macrophages, which possess an inflammatory phenotype and secrete large amounts of proteases, inflammatory cytokines, reactive radicals, and auto-and paracrine signaling molecules [227][228][229]. These "flaring" molecules drive lesion remodeling, invasiveness (and metastasis in the case of cancer), and can induce a phenotypical change in preexisting macrophages and other cells [230][231][232]. Thus, preventing macrophage activation and dampening local inflammation by using nanomedicines to deliver anti-inflammatory drugs can induce a favorable phenotype [233].…”

Section: The Proinflammatory Milieu and Local Cell Proliferationmentioning

confidence: 99%

Targeted therapeutics in inflammatory atherosclerosis

Alaarg¹

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Network dynamics determine the autocrine and paracrine signaling functions of TNF

Cited by 84 publications

References 64 publications

Effects of anti-inflammatory drugs on the expression of tryptophan-metabolism genes by human macrophages

Effects of anti-inflammatory drugs on the expression of tryptophan-metabolism genes by human macrophages

Deciphering the genomic toolkit underlying animal-bacteria interactions – insights through the demosponge Amphimedon queenslandica

Targeted therapeutics in inflammatory atherosclerosis

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