Inactivation of the Cerebral NFκB Pathway Inhibits Interleukin-1β-Induced Sickness Behavior and c-Fos Expression in Various Brain Nuclei

Nadjar, Agnès; Bluthé, Rose Marie; May, Michael J.; Dantzer, Robert; Parnet, Patricia

doi:10.1038/sj.npp.1300755

Cited by 108 publications

(64 citation statements)

References 44 publications

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“…Firstly, the SERT gene promoter is known to contain a consensus NF-jB binding site, suggesting that this transcription factor may be involved in the regulation of SERT gene expression in response to inflammatory stimulation [49]. Also, this transcription factor has previously been implicated in the precipitation of the clinical manifestation of sickness behavior as blockade of NF-jB activation following peripheral administration of IL-1b has been shown to attenuate the depressive-like behavioral effects of this peripherally administered cytokine in experimental animals [50]. Finally, the stimulation of both, primary astrocytes and C6 glioma cells, with TNF-a results in the activation of the NF-jB signaling pathway [40,51,52].…”

Section: Discussionmentioning

confidence: 99%

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The Pro-inflammatory Cytokine TNF-α Regulates the Activity and Expression of the Serotonin Transporter (SERT) in Astrocytes

et al. 2013

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Pro-inflammatory cytokines have been implicated in the precipitation of depression and related disorders, and the antidepressant sensitive serotonin transporter (SERT) may be a major target for immune regulation in these disorders. Here, we focus on astrocytes, a major class of immune competent cells in the brain, to examine the effects of pro-longed treatment with tumor necrosis factoralpha (TNF-a) on SERT activity. We first established that high-affinity serotonin uptake into C6 glioma cells occurs through a SERT-dependent mechanism. Functional SERT expression is also confirmed for primary astrocytes. In both cell types, exposure to TNF-a resulted in a dose-and timedependent increase in SERT-mediated 5-HT uptake, which was sustained for at least 48 h post-stimulation. Further analysis in primary astrocytes revealed that TNF-a enhanced the transport capacity (V max ) of SERT-specific 5-HT uptake, suggesting enhanced transporter expression, consistent with our observation of an increase in SERT mRNA levels. We confirmed that in both, primary astrocytes and C6 glioma cells, treatment with TNF-a activates the p38 mitogen-activated protein kinase (MAPK) signaling pathway. Pre-treatment with the p38 MAPK inhibitor SB203580 attenuated the TNF-a mediated stimulation of 5-HT transport in both, C6 glioma and primary astrocytes. In summary, we show that SERT gene expression and activity in astrocytes is subject to regulation by TNF-a, an effect that is at least in part dependent on p38 MAPK activation.

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Section: Discussionmentioning

confidence: 99%

“…1b). Using 50nM [ 3 H]5-HT, we obtained average IC 50 values for three well characterized SERT inhibitors: paroxetine, 0.66 ± 0.14 nM; escitalopram, 1.2 ± 0.35 nM; imipramine, 35.4 ± 1.6 nM. These values as well as the order of potency of these inhibitors, i.e.…”

Section: High-affinity 5-ht Uptake In C6 Glioma Cells Is Mediated By mentioning

confidence: 99%

The Pro-inflammatory Cytokine TNF-α Regulates the Activity and Expression of the Serotonin Transporter (SERT) in Astrocytes

et al. 2013

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“…The absence of MyD88 signalling has recently been shown to completely eliminate anorexia in response to either LPS or IL-1b . Interference with NF-kB production has also been shown to block the feeding-inhibitory effect of IL-1b (Nadjar et al 2005) and is the most likely mechanism by which genetic lack of PPARb, administration of phosphodiesterase inhibitors such as pentoxifylline (Porter et al 2000) and some other pharmacological interventions antagonize the feeding-inhibitory effect of LPS (for review, see Langhans, 2004). The neural mechanism(s) that mediate these effects, however, have not yet been determined.…”

Section: Lipopolysaccharide Receptor Mechanismsmentioning

confidence: 99%

Signals generating anorexia during acute illness

Langhans

2007

Proc. Nutr. Soc.

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Anorexia is part of the body's acute-phase response to illness. Microbial products such as lipopolysaccharides (LPS), which are also commonly used to model acute illness, trigger the acute-phase response and cause anorexia mainly through pro-inflammatory cytokines. LPS stimulate cytokine production through the cell-surface structural molecule CD14 and toll-like receptor-4. Cytokines ultimately change neural activity in brain areas controlling food intake and energy balance. The blood-brain barrier endothelial cells (BBB EC) are an important site of cytokine action in this context. BBB EC and perivascular cells (microglia and macrophages) form a complex regulatory interface that modulates neuronal activity by the release of messengers (e.g. PG, NO) in response to peripheral challenges. Serotonergic neurons originating in the raphe nuclei and glucagon-like peptide-1-expressing neurons in the hindbrain may be among the targets of these messengers, because serotonin (5-HT), acting through the 5-HT 2C receptor, and glucagon-like peptide-1 have recently emerged as neurochemical mediators of LPS anorexia. The central melanocortin system, which is a downstream target of serotonergic neurons, also appears to be involved in mediation of LPS anorexia. Interestingly, LPS also reduce orexin expression and the activity of orexin neurons in the lateral hypothalamic area of fasted mice. As the eating-stimulatory properties of orexin are apparently related to arousal, the inhibitory effect of LPS on orexin neurons might be involved in LPS-induced inactivity and anorexia. In summary, the immune signalling pathways of LPS-induced, and presumably acute illness-induced, anorexia converge on central neural signalling systems that control food intake and energy balance in healthy individuals.

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“…Michael May (Philadelphia, Pennsylvania) reported on the ability to specifically block the activation of this pathway upstream of NFκB activation, at the level of the IκB-kinase complex, using an inhibitor of the regulatory protein NEMO (NFκB essential modifier) coupled to a cell permeable peptide (May et al, 2000). Such blockade abrogates inflammation in various in vivo animal models, including cytokine-induced sickness behavior (Nadjar et al, 2005). Activation of stress-activated protein/mitogenactivated protein kinase (SAPK/MAPK) pathways also plays an important role in inflammation.…”

Section: Identification Of Possible Targets For Interventionmentioning

confidence: 99%

Identification and treatment of symptoms associated with inflammation in medically ill patients

Dantzer

Capuron

Irwin

et al. 2008

Psychoneuroendocrinology

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Medically ill patients present with a high prevalence of non-specific comorbid symptoms including pain, sleep disorders, fatigue and cognitive and mood alterations that is a leading cause of disability. However, despite major advances in the understanding of the immune-to-brain communication pathways that underlie the pathophysiology of these symptoms in inflammatory conditions, little has been done to translate this newly acquired knowledge to the clinics and to identify appropriate therapies. In a multidisciplinary effort to address this problem, clinicians and basic scientists with expertise in areas of inflammation, psychiatry, neurosciences and psychoneuroimmunology were brought together in a specialized meeting organized in Bordeaux, France, on May 28-29, 2007. These experts considered key questions in the field, in particular those related to identification and quantification of the predominant symptoms associated with inflammation, definition of systemic and central markers of inflammation, possible domains of intervention for controlling inflammation associated symptoms, and relevance of animal models of inflammation associated symptoms. This

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Inactivation of the Cerebral NFκB Pathway Inhibits Interleukin-1β-Induced Sickness Behavior and c-Fos Expression in Various Brain Nuclei

Cited by 108 publications

References 44 publications

The Pro-inflammatory Cytokine TNF-α Regulates the Activity and Expression of the Serotonin Transporter (SERT) in Astrocytes

The Pro-inflammatory Cytokine TNF-α Regulates the Activity and Expression of the Serotonin Transporter (SERT) in Astrocytes

Signals generating anorexia during acute illness

Identification and treatment of symptoms associated with inflammation in medically ill patients

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