Neural activities of IL‐6‐type cytokines often depend on soluble cytokine receptors

März, Pia; Otten, U.; Rose-John, Stefan

doi:10.1046/j.1460-9568.1999.00755.x

Cited by 119 publications

(76 citation statements)

References 110 publications

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“…Because IL-1␤ and TNF␣ share a number of biological properties, common signaling may be assumed that may involve receptor-associated kinases. This would be in line with a pronounced sensitization of heat-activated ion channels by phosphorylation (Cesare and McNaughton, 1996;März et al, 1999).…”

Section: Discussionsupporting

confidence: 62%

“…The additional presence of soluble IL-6 receptor is required, and this may represent dual regulation of IL-6 signaling by the cytokine and its receptor. From other models it is known that neural activities of IL-6-like cytokines often depend on soluble receptor (März et al, 1999). A potential role for IL-6 in the inflammatory heat hyperalgesia is further supported by a recent report of a reduced heat sensitivity in IL-6 null mutant mice in the hot plate test (Zhong et al, 1999).…”

Section: Discussionmentioning

confidence: 89%

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Involvement of the Proinflammatory Cytokines Tumor Necrosis Factor-α, IL-1β, and IL-6 But Not IL-8 in the Development of Heat Hyperalgesia: Effects on Heat-Evoked Calcitonin Gene-Related Peptide Release from Rat Skin

2000

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Proinflammatory cytokines contribute to the development of inflammatory and neuropathic pain and hyperalgesia in many in vivo models. The rat skin model was used to investigate the effects of proinflammatory cytokines on the basal and heatevoked release of calcitonin gene-related peptide from nociceptors in vitro. In contrast to the excitatory effects of cytokines observed in vivo, none of the cytokines tested evoked any calcitonin gene-related peptide (CGRP) release at normal skin temperature of 32°C. However, the cytokines IL-1␤, tumor necrosis factor (TNF)-␣, and IL-6 but not IL-8 induced a pronounced and transient sensitization of the heat-evoked CGRP release from nociceptors in vitro. This heat sensitization was dose dependent, with EC 50 for IL-1␤ of 2.7 ng/ml and for TNF-␣ of 3.1 ng/ml. The maximum IL-1␤ effect reached almost 600% of the heat-evoked release, and the maximum TNF-␣ effect induced a rise in CGRP release of 350%. In contrast to IL-1␤ and TNF-␣, IL-6 did not induce heat sensitization when applied alone but was only effective in the presence of soluble IL-6 receptor. This suggests a constitutive expression of signaling receptors for TNF and IL-1␤ and the signal transduction molecule gp130 but not IL-6 receptor or IL-8 receptor. Furthermore, the acute cytokine signaling observed in the present study was independent of transcriptional pathways because sensitization occurred on short latency in vitro and under conditions that excluded chemotactic accumulation of immune cells from blood vessels. Our results demonstrate that interleukins may play an important role in the initiation of heat hyperalgesia in inflammation and neuropathy.

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Section: Discussionsupporting

confidence: 62%

Section: Discussionmentioning

confidence: 89%

Involvement of the Proinflammatory Cytokines Tumor Necrosis Factor-α, IL-1β, and IL-6 But Not IL-8 in the Development of Heat Hyperalgesia: Effects on Heat-Evoked Calcitonin Gene-Related Peptide Release from Rat Skin

2000

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“…The principle of trans-signaling via sIL-6R enlarges the spectrum of IL-6 target cells, among them rat sympathetic and DRG neurons (Jones et al 2005;Rose-John et al 2007). From previous studies in our laboratory, it is known that rat sympathetic neurons contain only a marginal number of membrane-bound IL-6 receptors and strongly respond to IL-6 via trans-signaling (März et al 1998(März et al , 1999. In vivo, plasma levels of sIL-6R in healthy individuals were found to be in the range of about 25-35 ng/ml and elevated levels associated with numerous inflammatory disease states such as Crohn's disease, rheumatoid arthritis (RA), juvenile RA, and osteoarthritis (Rose-John et al 2007).…”

Section: Discussionmentioning

confidence: 99%

Expression of Pancreatitis-Associated Protein after Traumatic Brain Injury: A Mechanism Potentially Contributing to Neuroprotection in Human Brain

März-Weiss

Kunz

Bimmler³

et al. 2011

Cell Mol Neurobiol

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Neuronal cell death after severe traumatic brain injury (TBI) is caused by a complex interplay of pathological mechanisms including excitotoxicity, oxidative stress, mitochondrial dysfunction, extensive neuroinflammation, and ischemia-reperfusion injury. Pancreatitis-associated protein I (PAP I/reg2) was reported to be a survival factor for peripheral neurons, particularly sensory and motor neurons. In rat brains, by experimental TBI as well as by kainic acid induced brain seizure, PAP I and PAP III were found to be up-regulated in central neurons. In this study, we performed immunohistochemical staining in postmortem human brain from patients who died after severe TBI to demonstrate PAP expression on protein level in cerebellar Purkinje cells, pyramidal and granular neurons in cerebral cortex, and cortical neurons in the fore-and mid-brain. In primary cultures of rat brain cortical, hippocampal, and cerebellar neurons, we found neuroprotective effects for PAP I on H 2 O 2 -induced oxidative stress. Moreover, serum K ? -deprivation induces apoptotic cell death in 55% of cerebellar granule neurons (CGN), whereas upon treatment with PAP I only 32% of CGN are apoptotic. Using Western blot analyses, we compared protein phosphorylation in neuronal signaling pathways activated by PAP I versus Interleukin-6 (IL-6). We found a rapid activation of Akt-kinase phosphorylation by PAP I with a peak at 15 min, whereas IL-6 induces Akt-phosphorylation lasting longer than 30 min. Phosphorylation of MAP-42/44 kinases is stimulated in a comparable fashion. Both, IL-6 and PAP I increase phosphorylation of NFjB for activation of gene transcription, whereas only IL-6 recruits STAT3 phosphorylation, indicating that STAT3 is not a target of PAP I transcription activation in brain neurons. Application of the Akt-inhibitor Wortmanin reveals only a partial inhibition of PAP I-dependent protection of CGN from H 2 O 2 -induced oxidative stress. Based on our findings, we suggest that PAP I is a long lasting neurotrophic signal for central neurons. The neuroprotective effects parallel those that have been Pia März-Weiss and Dieter Kunz contributed equally in this study.Electronic supplementary material The online version of this article

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“…The glycosyl phosphatidylinositol linkage of CNTFR␣ to the cell membrane can be cleaved by phospholipases releasing CNTFR␣ to act as a soluble protein (Taga et al, 1989). Although most soluble receptors for cytokines and growth factors act antagonistically with their membrane-bound counterparts, soluble CNTFR␣ retains its ability to bind CNTF and act as an agonistic autocrine or paracrine factor (Marz et al, 1999). The heterodimer of CNTF and soluble CNTFR␣ (hereinafter termed "Complex") can trans-signal cells, independent of endogenous CNTFR␣ expression, by binding with the required ␤ subunits glycoprotein 130 (gp130) and leukemia inhibitory factor receptor ␤ (LIFR␤) (Davis et al, 1993a;Rose-John and Heinrich, 1994;Stahl et al, 1994).…”

Section: Introductionmentioning

confidence: 99%

The Complex of Ciliary Neurotrophic Factor-Ciliary Neurotrophic Factor Receptor α Up-Regulates Connexin43 and Intercellular Coupling in Astrocytes via the Janus Tyrosine Kinase/Signal Transducer and Activator of Transcription Pathway

Ozog

Bernier

Bates

et al. 2004

MBoC

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Cytokines regulate numerous cell processes, including connexin expression and gap junctional coupling. In this study, we examined the effect of ciliary neurotrophic factor (CNTF) on connexin43 (Cx43) expression and intercellular coupling in astrocytes. Murine cortical astrocytes matured in vitro were treated with CNTF (20 ng/ml), soluble ciliary neurotrophic factor receptor ␣ (CNTFR␣) (200 ng/ml), or CNTF-CNTFR␣. Although CNTF and CNTFR␣ alone had no effect on Cx43 expression, the heterodimer CNTF-CNTFR␣ significantly increased both Cx43 mRNA and protein levels. Cx43 immunostaining correlated with increased intercellular coupling as determined by dye transfer analysis. By using the pharmacological inhibitor ␣-cyano-(3,4-dihydroxy)-N-benzylcinnamide (AG490), the increase in Cx43 was found to be dependent on the Janus tyrosine kinase/signal transducer and activator of transcription (JAK/STAT) pathway. Immunocytochemical analysis revealed that CNTF-CNTFR␣ treatment produced nuclear localization of phosphorylated STAT3, whereas CNTF treatment alone did not. Transient transfection of constructs containing various sequences of the Cx43 promoter tagged to a LacZ reporter into ROS 17/2.8 cells confirmed that the promoter region between ؊838 to ؊1693 was deemed necessary for CNTF-CNTFR␣ to induce heightened expression. CNTF-CNTFR␣ did not alter Cx30 mRNA levels, suggesting selectivity of CNTF-CNTFR␣ for connexin signaling. Together in the presence of soluble receptor, CNTF activates the JAK/STAT pathway leading to enhanced Cx43 expression and intercellular coupling. INTRODUCTIONGap junctions are intercellular channels between adjacent cells that permit the passage of various substances Ͻ1.2 kDa in size (Kumar and Gilula, 1996). Such junctions are formed when each cell provides a connexon, which itself is composed of six connexins (Cxs) (Kumar and Gilula, 1996). Cx43, the prominent Cx isoform expressed in the central nervous system (CNS), is highly expressed in astrocytes (Yamamoto et al., 1990;Dermietzel et al., 1991;Giaume et al., 1991), neuronal precursors (Rozental et al., 1998Bittman and LoTurco, 1999), and possibly neurons (Bruzzone and Ressot, 1997;Vaney, 1999;SiuYi et al., 2001;Rouach et al., 2002). Several studies using in vitro and in vivo models have demonstrated that impediment of gap junctional coupling and/or connexin43 expression amplifies cell death and tissue damage in the wake of injuries and diseases (Blanc et al., 1998;Naus et al., 2001;Siushansian et al., 2001;Ozog et al., 2002b;Lin et al., 2003;Nakase et al., 2003). Thus, design of an intervention to up-regulate Cx43 expression and intercellular communication may lead to novel therapies against pathological disturbances.Gap junction expression and activity can be altered on a short-term or long-term basis (reviewed by Giaume and McCarthy, 1996;Rouach and Giaume, 2001). Short-term regulation is the result of posttranslational processing such as phosphorylation or channel blocking. Long-term regulation, however, entails modification of gene transcripti...

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Neural activities of IL‐6‐type cytokines often depend on soluble cytokine receptors

Cited by 119 publications

References 110 publications

Involvement of the Proinflammatory Cytokines Tumor Necrosis Factor-α, IL-1β, and IL-6 But Not IL-8 in the Development of Heat Hyperalgesia: Effects on Heat-Evoked Calcitonin Gene-Related Peptide Release from Rat Skin

Involvement of the Proinflammatory Cytokines Tumor Necrosis Factor-α, IL-1β, and IL-6 But Not IL-8 in the Development of Heat Hyperalgesia: Effects on Heat-Evoked Calcitonin Gene-Related Peptide Release from Rat Skin

Expression of Pancreatitis-Associated Protein after Traumatic Brain Injury: A Mechanism Potentially Contributing to Neuroprotection in Human Brain

The Complex of Ciliary Neurotrophic Factor-Ciliary Neurotrophic Factor Receptor α Up-Regulates Connexin43 and Intercellular Coupling in Astrocytes via the Janus Tyrosine Kinase/Signal Transducer and Activator of Transcription Pathway

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