Your search keyword '"Siegmund, Daniela"' showing total 13 results

1. Membrane lymphotoxin-α 2 β is a novel tumor necrosis factor (TNF) receptor 2 (TNFR2) agonist.

Author

Kucka K, Lang I, Zhang T, Siegmund D, Medler J, and Wajant H

Subjects

Humans, Membranes metabolism, Receptors, Tumor Necrosis Factor, Type I agonists, Receptors, Tumor Necrosis Factor, Type I drug effects, Receptors, Tumor Necrosis Factor, Type I metabolism, Signal Transduction immunology, Lymphotoxin-alpha metabolism, Receptors, Tumor Necrosis Factor, Type II agonists, Receptors, Tumor Necrosis Factor, Type II metabolism, Signal Transduction physiology, Tumor Necrosis Factor-alpha metabolism

Abstract

In the early 1990s, it has been described that LTα and LTβ form LTα 2 β and LTαβ 2 heterotrimers, which bind to TNFR1 and LTβR, respectively. Afterwards, the LTαβ 2 -LTβR system has been intensively studied while the LTα 2 β-TNFR1 interaction has been ignored to date, presumably due to the fact that at the time of identification of the LTα 2 β-TNFR1 interaction one knew already two ligands for TNFR1, namely TNF and LTα. Here, we show that LTα 2 β interacts not only with TNFR1 but also with TNFR2. We furthermore demonstrate that membrane-bound LTα 2 β (memLTα 2 β), despite its asymmetric structure, stimulates TNFR1 and TNFR2 signaling. Not surprising in view of its ability to interact with TNFR2, LTα 2 β is inhibited by Etanercept, which is approved for the treatment of rheumatoid arthritis and also inhibits TNF and LTα.

Published

2021

2. Redundant and receptor-specific activities of TRADD, RIPK1 and FADD in death receptor signaling.

Author

Füllsack S, Rosenthal A, Wajant H, and Siegmund D

Subjects

Apoptosis drug effects, Caspase 8 metabolism, HeLa Cells, Humans, NF-kappa B metabolism, Oligopeptides pharmacology, Receptor-Interacting Protein Serine-Threonine Kinases deficiency, Receptor-Interacting Protein Serine-Threonine Kinases genetics, TNF-Related Apoptosis-Inducing Ligand pharmacology, Tumor Necrosis Factor-alpha pharmacology, Fas-Associated Death Domain Protein metabolism, Receptor-Interacting Protein Serine-Threonine Kinases metabolism, Signal Transduction drug effects, TNF Receptor-Associated Death Domain Protein metabolism

Abstract

We evaluated redundant and receptor-specific activities of TRADD, RIPK1, and FADD in RIPK3-expressing HeLa cells lacking expression of these proteins or any combination of two of these factors. We confirmed the opposing role of FADD in TNF- and TRAIL-induced necroptosis and observed an anti-necroptotic function of TRADD. RIPK1 and TRADD act in a redundant manner in TNF- but not TRAIL-induced apoptosis. Complementary, FADD proved to be sufficient for TRAIL- but not for TNF-induced apoptosis. TRADD and RIPK1, however, redundantly mediated proinflammatory signaling in response to TNF and TRAIL. FADD deficiency sensitized more efficiently for TNFR1-mediated necroptosis than caspase-8 deficiency pointing to a caspase-8 independent inhibitory activity of FADD on TNF-induced necroptosis. Based on these characteristics, we propose a model in which the death receptor-specific activities of TRADD, RIPK1, and FADD are traced back to their hierarchically different position in TNFR1- and TRAIL death receptor signaling.

Published

2019

3. TWEAK inhibits TRAF2-mediated CD40 signaling by destabilization of CD40 signaling complexes.

Author

Salzmann S, Lang I, Rosenthal A, Schäfer V, Weisenberger D, Carmona Arana JA, Trebing J, Siegmund D, Neumann M, and Wajant H

Subjects

Blotting, Western, CD40 Antigens immunology, CD40 Ligand immunology, Cell Line, Cytokine TWEAK, Flow Cytometry, Humans, Immunoprecipitation, Microscopy, Confocal, Receptors, Tumor Necrosis Factor immunology, TNF Receptor-Associated Factor 2 immunology, TWEAK Receptor, Tumor Necrosis Factors immunology, CD40 Antigens metabolism, CD40 Ligand metabolism, Receptors, Tumor Necrosis Factor metabolism, Signal Transduction physiology, TNF Receptor-Associated Factor 2 metabolism, Tumor Necrosis Factors metabolism

Abstract

We found recently that TNF-like weak inducer of apoptosis (TWEAK) and fibroblast growth factor-inducible-14 (Fn14) by virtue of their strong capability to reduce the freely available cytoplasmic pool of TNFR-associated factor (TRAF)2 and cellular inhibitors of apoptosis (cIAPs) antagonize the functions of these molecules in TNFR1 signaling, resulting in sensitization for apoptosis and inhibition of classical NF-κB signaling. In this study, we demonstrate that priming of cells with TWEAK also interferes with activation of the classical NF-κB pathway by CD40. Likewise, there was strong inhibition of CD40 ligand (CD40L)-induced activation of MAPKs in TWEAK-primed cells. FACS analysis and CD40L binding studies revealed unchanged CD40 expression and normal CD40L-CD40 interaction in TWEAK-primed cells. CD40L immunoprecipitates, however, showed severely reduced amounts of CD40 and CD40-associated proteins, indicating impaired formation or reduced stability of CD40L-CD40 signaling complexes. The previously described inhibitory effect of TWEAK on TNFR1 signaling has been traced back to reduced activity of the TNFR1-associated TRAF2-cIAP1/2 ubiquitinase complex and did not affect the stability of the immunoprecipitable TNFR1 receptor complex. Thus, the inhibitory effect of TWEAK on CD40 signaling must be based at least partly on other mechanisms. In line with this, signaling by the CD40-related TRAF2-interacting receptor TNFR2 was also attenuated but still immunoprecipitable in TWEAK-primed cells. Collectively, we show that Fn14 activation by soluble TWEAK impairs CD40L-CD40 signaling complex formation and inhibits CD40 signaling and thus identify the Fn14-TWEAK system as a potential novel regulator of CD40-related cellular functions.

Published

2013

4. Fibroblast growth factor inducible (Fn14)-specific antibodies concomitantly display signaling pathway-specific agonistic and antagonistic activity.

Author

Salzmann S, Seher A, Trebing J, Weisenberger D, Rosenthal A, Siegmund D, and Wajant H

Subjects

Amino Acid Substitution, Animals, Antibodies, Monoclonal chemistry, Antibodies, Monoclonal, Humanized chemistry, Bacterial Proteins chemistry, Cell Line, Tumor, Cytokine TWEAK, Endonucleases, HEK293 Cells, Humans, Interleukin-8 biosynthesis, Macaca fascicularis, Mice, Mutagenesis, Site-Directed, NF-kappa B metabolism, Nuclear Proteins metabolism, Protein Binding, Protein Multimerization, Receptors, IgG agonists, Receptors, IgG metabolism, Receptors, Tumor Necrosis Factor genetics, Receptors, Tumor Necrosis Factor metabolism, TWEAK Receptor, Tumor Necrosis Factor Inhibitors, Tumor Necrosis Factor-alpha physiology, Tumor Necrosis Factors physiology, Antibodies, Monoclonal pharmacology, Antibodies, Monoclonal, Humanized pharmacology, Receptors, Tumor Necrosis Factor immunology, Signal Transduction drug effects

Abstract

Background: Fn14 is a therapeutic target in various diseases., Results: Anti-Fn14 antibodies activate the alternative NFκB pathway but not other Fn14-related activities induced by soluble or membrane-bound TWEAK. FcγR-bound anti-Fn14 antibodies, however, activate the full spectrum of Fn14-associated activities., Conclusion: Anti-Fn14 antibodies elicit agonistic activities differing from those of the natural Fn14 ligand TWEAK., Significance: These findings influence the rationale of designing Fn14-targeted therapies. The Fn14-specific monoclonal antibodies PDL192 and P4A8, which are under consideration in clinical trials, showed no agonistic activity with respect to IL8 production and cell death induction. However, oligomerization with protein G or binding to Fcγ receptors converted both anti-Fn14 antibodies into potent agonists. TNF-like weak inducer of apoptosis (TWEAK), the ligand of Fn14, occurs naturally in two forms with partly different signaling capabilities, as a membrane-bound ligand and as a soluble trimeric molecule. Although membrane TWEAK strongly triggers all Fn14-associated pathways, soluble TWEAK predominately triggers the alternative nuclear factor κB (NFκB) pathway and enhances TNF-induced cell death but has only a poor effect on the classical NFκB pathway and chemokine production. Thus, the oligomerized and FcγR-bound anti-Fn14 mAbs mimicked the activity of membrane TWEAK. Notably, both anti-Fn14 antibodies significantly triggered p100 processing, the hallmark of the alternative NFκB pathway, and therefore resembled soluble TWEAK. In contrast to the latter, however, the anti-Fn14s showed no effect on TNF receptor 1-induced cell death and P4A8 even blocked the corresponding TWEAK response. Thus, we showed that Fn14 antibodies display an alternative NFκB pathway-specific agonistic activity but fail to phenocopy other activities of soluble TWEAK, whereas oligomerized or FcγR-bound Fn14 antibodies fully mimic the activity of membrane TWEAK. In view of the trivalent nature of the TWEAK-Fn14 interaction, this suggests that the alternative NFκB pathway is uniquely responsive already to Fn14 dimerization enabling antibodies to elicit an unnatural response pattern distinct from that of the naturally occurring Fn14 ligands.

Published

2013

5. The IKK inhibitor Bay 11-7082 induces cell death independent from inhibition of activation of NFκB transcription factors.

Author

Rauert-Wunderlich H, Siegmund D, Maier E, Giner T, Bargou RC, Wajant H, and Stühmer T

Subjects

Amides pharmacology, Blotting, Western, Cell Line, Cell Survival drug effects, Cyclopentanes pharmacology, Enzyme-Linked Immunosorbent Assay, Flow Cytometry, Gene Expression Regulation, Neoplastic drug effects, Humans, Microscopy, Fluorescence, Pyrimidines pharmacology, RNA, Small Interfering genetics, Signal Transduction drug effects, Thiophenes pharmacology, Apoptosis drug effects, Gene Expression Regulation, Neoplastic genetics, I-kappa B Kinase antagonists & inhibitors, Multiple Myeloma metabolism, NF-kappa B metabolism, Nitriles pharmacology, Signal Transduction genetics, Sulfones pharmacology

Abstract

Multiple myeloma (MM) displays an NFκB activity-related gene expression signature and about 20% of primary MM samples harbor genetic alterations conducive to intrinsic NFκB signaling activation. The relevance of blocking the classical versus the alternative NFκB signaling pathway and the molecular execution mechanisms involved, however, are still poorly understood. Here, we comparatively tested NFκB activity abrogation through TPCA-1 (an IKK2 inhibitor), BAY 11-7082 (an IKK inhibitor poorly selective for IKK1 and IKK2), and MLN4924 (an NEDD8 activating enzyme (NAE)-inhibitor), and analyzed their anti-MM activity. Whereas TPCA-1 interfered selectively with activation of the classical NFκB pathway, the other two compounds inhibited classical and alternative NFκB signaling without significant discrimination. Noteworthy, whereas TPCA-1 and MLN4924 elicited rather mild anti-MM effects with slight to moderate cell death induction after 1 day BAY 11-7082 was uniformly highly toxic to MM cell lines and primary MM cells. Treatment with BAY 11-7082 induced rapid cell swelling and its initial effects were blocked by necrostatin-1 or the ROS scavenger BHA, but a lasting protective effect was not achieved even with additional blockade of caspases. Because MLN4924 inhibits the alternative NFκB pathway downstream of IKK1 at the level of p100 processing, the quite discordant effects between MLN4924 and BAY 11-7082 must thus be due to blockade of IKK1-mediated NFκB-independent necrosis-inhibitory functions or represent an off-target effect of BAY 11-7082. In accordance with the latter, we further observed that concomitant knockdown of IKK1 and IKK2 did not have any major short-term adverse effect on the viability of MM cells.

Published

2013

6. Signaling active CD95 receptor molecules trigger co-translocation of inactive CD95 molecules into lipid rafts.

Author

Lang I, Fick A, Schäfer V, Giner T, Siegmund D, and Wajant H

Subjects

Apoptosis drug effects, Blotting, Western, CD40 Antigens chemistry, CD40 Antigens genetics, CD40 Antigens metabolism, Cell Line, Cell Line, Tumor, Cycloheximide pharmacology, Fas Ligand Protein chemistry, Fas Ligand Protein genetics, HEK293 Cells, Humans, Jurkat Cells, Kinetics, Membrane Proteins chemistry, Membrane Proteins genetics, Membrane Proteins metabolism, Mutation, Protein Binding drug effects, Protein Multimerization, Protein Synthesis Inhibitors pharmacology, Protein Transport, Solubility, fas Receptor chemistry, fas Receptor genetics, Fas Ligand Protein metabolism, Membrane Microdomains metabolism, Signal Transduction, fas Receptor metabolism

Abstract

The capability of soluble CD95L trimers to trigger CD95-associated signaling pathways is drastically increased by oligomerization. The latter can be achieved, for example, by antibodies recognizing a N-terminal epitope tag in recombinant CD95L variants or by genetic engineering-enforced formation of hexamers. Using highly sensitive and accurate binding studies with recombinant CD95L variants equipped with a Gaussia princeps luciferase reporter domain, we found that oligomerization of CD95L has no major effect on CD95 occupancy. This indicates that the higher activity of oligomerized CD95L trimers is not related to an avidity-related increase in apparent affinity and points instead to a crucial role of aggregation of initially formed trimeric CD95L-CD95 complexes in CD95 activation. Furthermore, binding of soluble CD95L trimers was found to be insufficient to increase the association of CD95 with the lipid raft-containing membrane fraction. However, when Gaussia princeps luciferase-CD95L trimers were used as tracers to "mark" inactive CD95 molecules, increased association of these inactive receptors was observed upon activation of the remaining CD95 molecules by help of highly active hexameric Fc-CD95L or membrane CD95L. Moreover, in cells expressing endogenous CD95 and chimeric CD40-CD95 receptors, triggering of CD95 signaling via endogenous CD95 resulted in co-translocation of CD40-CD95 to the lipid raft fraction, whereas vice versa activation of CD95-associated pathways with Fc-CD40L via CD40-CD95 resulted in co-translocation of endogenous CD95. In sum, this shows that signaling-active CD95 molecules not only enhance their own association with the lipid raft-containing membrane fraction but also those of inactive CD95 molecules.

Published

2012

7. Membrane tumor necrosis factor (TNF) induces p100 processing via TNF receptor-2 (TNFR2).

Author

Rauert H, Wicovsky A, Müller N, Siegmund D, Spindler V, Waschke J, Kneitz C, and Wajant H

Subjects

Active Transport, Cell Nucleus physiology, Animals, Cell Line, Tumor, Cells, Cultured, Humans, NF-kappa B p52 Subunit genetics, Protein Isoforms genetics, Protein Isoforms metabolism, Protein Subunits genetics, Protein Subunits metabolism, Receptors, Tumor Necrosis Factor, Type I genetics, Receptors, Tumor Necrosis Factor, Type I metabolism, Receptors, Tumor Necrosis Factor, Type II genetics, T-Lymphocytes cytology, T-Lymphocytes metabolism, Transcription Factor RelB genetics, Transcription Factor RelB metabolism, Tumor Necrosis Factors genetics, NF-kappa B p52 Subunit metabolism, Receptors, Tumor Necrosis Factor, Type II metabolism, Signal Transduction physiology, Tumor Necrosis Factors metabolism

Abstract

Tumor necrosis factor (TNF) elicits its biological activities by stimulation of two receptors, TNFR1 and TNFR2, both belonging to the TNF receptor superfamily. Whereas TNFR1-mediated signal transduction has been intensively studied and is understood in detail, especially with respect to activation of the classical NFkappaB pathway, cell death induction, and MAP kinase signaling, TNFR2-associated signal transduction is poorly defined. Here, we demonstrate in various tumor cell lines and primary T-cells that TNFR2, but not TNFR1, induces activation of the alternative NFkappaB pathway. In accord with earlier findings demonstrating that only membrane TNF, but not soluble TNF, properly activates TNFR2, we further show by use of TNFR1- and TNFR2-specific mutants of soluble TNF and membrane TNF that soluble ligand trimers fail to activate the alternative NFkappaB pathway. In accord with the known inhibitory role of TRAF2 in the alternative NFkappaB pathway, TNFR2-, but not TNFR1-specific TNF induced depletion of cytosolic TRAF2. Thus, we identified activation of the alternative NFkappaB pathway as a TNF signaling effect that can be specifically assigned to TNFR2 and membrane TNF.

Published

2010

8. Oligomerized tumor necrosis factor-related apoptosis inducing ligand strongly induces cell death in myeloma cells, but also activates proinflammatory signaling pathways.

Author

Berg D, Stühmer T, Siegmund D, Müller N, Giner T, Dittrich-Breiholz O, Kracht M, Bargou R, and Wajant H

Subjects

Amino Acid Chloromethyl Ketones pharmacology, Caspase Inhibitors, Caspases metabolism, Cell Death, Cell Line, Tumor, Humans, JNK Mitogen-Activated Protein Kinases metabolism, Multiple Myeloma enzymology, Multiple Myeloma pathology, NF-kappa B metabolism, Apoptosis, Inflammation Mediators metabolism, Multiple Myeloma metabolism, Signal Transduction, TNF-Related Apoptosis-Inducing Ligand metabolism

Abstract

The oligomerization status of soluble tumor necrosis factor-related apoptosis inducing ligand (TRAIL) trimers has an overwhelming impact on cell death induction in a cell-type dependent fashion. Thus, we evaluated the ability of single and oligomerized TRAIL trimers to induce cell death in human myeloma cells. In all myeloma cell lines analyzed, oligomerized TRAIL trimers induced caspase activation and complete cell death, whereas non-oligomerized TRAIL trimers showed no or only a modest effect. Caspase activation induced by oligomerized TRAIL was blocked in all cell lines by the pan-caspase inhibitor benzyloxycarbonyl-Val-Ala-Asp(OMe)-fluoromethylketone (z-VAD-fmk). Cell death induction was largely blocked in two cell lines by z-VAD-fmk, but was only marginally attenuated in three other cell lines, indicating that TRAIL induces caspase-dependent and caspase-independent cell death in myeloma cells. Preceding cell death, TRAIL activated nuclear factor kappaB, c-Jun N-terminal kinase, p38 and p42/44. Although TRAIL-induced stimulation of c-Jun N-terminal kinase and p38 was caspase-dependent in a cell type-specific fashion, activation of nuclear factor kappaB and p42/44 was caspase-independent in all cases. In accordance with activation of the nuclear factor kappaB pathway, we observed transcriptional up-regulation of several well established nuclear factor kappaB target genes. Furthermore, we found that TRAIL activates proinflammatory pathways in approximately 50% of primary myeloma samples. Taken together, our data suggest (a) that oligomerized TRAIL variants are necessary to ensure maximal cell death induction in myeloma cells and (b) TRAIL should be used in combination with anti-inflammatory drugs for treatment of myeloma to avoid and/or minimize any potential side-effects arising from the proinflammatory properties of the molecule.

Published

2009

9. Role of caspases in CD95L- and TRAIL-induced non-apoptotic signalling in pancreatic tumour cells.

Author

Siegmund D, Klose S, Zhou D, Baumann B, Röder C, Kalthoff H, Wajant H, and Trauzold A

Subjects

Amino Acid Chloromethyl Ketones pharmacology, CASP8 and FADD-Like Apoptosis Regulating Protein metabolism, Caspase 8 metabolism, Cell Line, Tumor, Enzyme Activation drug effects, Extracellular Signal-Regulated MAP Kinases metabolism, Humans, Inflammation Mediators metabolism, NF-kappa B metabolism, TNF Receptor-Associated Factor 2 metabolism, bcl-X Protein metabolism, Apoptosis drug effects, Caspases metabolism, Fas Ligand Protein pharmacology, Pancreatic Neoplasms enzymology, Pancreatic Neoplasms pathology, Signal Transduction drug effects, TNF-Related Apoptosis-Inducing Ligand pharmacology

Abstract

The CD95 and TRAIL death receptors can potently stimulate proinflammatory signalling, especially in apoptosis resistant cells. Here, we show that caspases are of cell type-specific relevance for non-apoptotic death receptor signalling in pancreatic tumour cells. Inhibition of caspases by zVAD-fmk strongly enhanced the proinflammatory response in PancTuI, BxPc3 and Panc89 cells, but inhibited this response in Colo357 cells as well as in apoptosis-resistant Colo357-BclxL cells overexpressing BclxL. To characterize the role of caspases in non-apoptotic death receptor signalling, we analysed CD95L- and TRAIL-induced signalling pathways in Colo357-BclxL cells in comparison with PancTuI cells. Both death ligands induced NFkappaB, ERKs, JNK and p38 in Colo357-BclxL cells and except for ERKs also in PancTuI cells. However, inhibition of caspases with zVAD-fmk resulted in strong inhibition of all these signalling pathways in Colo357-BclxL, but enhanced NFkappaB and JNK signalling in PancTuI cells. Caspase-mediated activation of NFkappaB and ERKs were involved in CD95L- and TRAIL-induced up-regulation of proinflammatory genes in Colo357-BclxL cells. At the level of the DISC we did not observe any significant differences in recruitment or processing of FADD, caspase-8, FLIP, TRAF2 and RIP between PancTuI and Colo357-BclxL cells. Consequently, an NFkappaB and ERK stimulating, caspase-dependent factor must operate downstream of the DISC in Colo357-BclxL cells.

Published

2007

10. A CD40-CD95L fusion protein interferes with CD40L-induced prosurvival signaling and allows membrane CD40L-restricted activation of CD95.

Author

Assohou-Luty C, Gerspach J, Siegmund D, Müller N, Huard B, Tiegs G, Pfizenmaier K, and Wajant H

Subjects

Animals, CD40 Antigens metabolism, CD40 Ligand metabolism, Cell Death, Cell Survival, Fas Ligand Protein metabolism, Humans, Mice, Mice, Inbred BALB C, Mice, Inbred C57BL, Protein Binding, Protein Structure, Tertiary, RANK Ligand metabolism, Receptor Activator of Nuclear Factor-kappa B metabolism, Receptors, TNF-Related Apoptosis-Inducing Ligand metabolism, Recombinant Fusion Proteins metabolism, TNF-Related Apoptosis-Inducing Ligand metabolism, fas Receptor metabolism, CD40 Antigens immunology, CD40 Ligand immunology, Cell Membrane metabolism, Fas Ligand Protein immunology, Signal Transduction, fas Receptor immunology

Abstract

We analyzed a novel bifunctional fusion protein, CD40ed-CD95Led, consisting amino-terminally of the extracellular domain of CD40 and carboxy-terminally of the extracellular domain of CD95L. On cells lacking CD40L, this fusion protein is poorly active with respect to CD95 activation [median effective dose (ED50)>1 microg/ml], but it stimulates CD95 signaling with high efficiency upon binding to membrane-expressed CD40L (ED50<1 ng/ml). Thus, cell surface immobilization mediated by the CD40 part of the molecule unmasks the high-latent, CD95-stimulating capacity of the otherwise poorly active CD95L fusion protein. Moreover, interaction of the CD40 part of CD40ed-CD95Led with CD40L prevents the activation of cellular CD40. The CD40ed-CD95Led fusion protein therefore simultaneously blocks antiapoptotic CD40 activation and induces CD95-mediated apoptosis. Indeed, T47D cells displaying an antiapoptotic autocrine CD40-CD40L signaling loop were significantly more sensitive toward CD40ed-CD95Led than toward soluble CD95L artificially activated by crosslinking. Fusion proteins of RANK and CD95L (RANKed-CD95Led) and CD40 and tumor necrosis factor-related apoptosis inducing ligand (TRAIL) (CD40ed-TRAILed), with domain architectures similar to CD40ed-Cd95Led, displayed RANKL-dependent CD95 and CD40L-dependent TRAILR2 activation, respectively, indicating the principle feasibility of this fusion protein design.

Published

2006

11. Death receptor-induced signaling pathways are differentially regulated by gamma interferon upstream of caspase 8 processing.

Author

Siegmund D, Wicovsky A, Schmitz I, Schulze-Osthoff K, Kreuz S, Leverkus M, Dittrich-Breiholz O, Kracht M, and Wajant H

Subjects

Apoptosis physiology, Caspase 8, Death Domain Receptor Signaling Adaptor Proteins, Fas Ligand Protein, Humans, KB Cells, Membrane Glycoproteins genetics, Mitogen-Activated Protein Kinases metabolism, NF-kappa B metabolism, Receptors, TNF-Related Apoptosis-Inducing Ligand, Caspases metabolism, Interferon-gamma physiology, Membrane Glycoproteins metabolism, Protein Processing, Post-Translational physiology, Receptors, Tumor Necrosis Factor metabolism, Signal Transduction physiology

Abstract

FasL and gamma interferon (IFN-gamma) are produced by activated T cells and NK cells and synergistically induce apoptosis. Although both cytokines can also elicit proinflammatory responses, a possible cross talk of these ligands with respect to nonapoptotic signaling has been poorly addressed. Here, we show that IFN-gamma sensitizes KB cells for apoptosis induction by facilitating death-inducing signaling complex (DISC)-mediated caspase 8 processing. Moreover, after protection against death receptor-induced apoptosis by caspase inhibition or Bcl2 overexpression, IFN-gamma also sensitized for Fas- and TRAIL death receptor-mediated NF-kappaB activation leading to synergistic upregulation of a variety of proinflammatory genes. In contrast, Fas-mediated activation of JNK, p38, and p42/44 occurred essentially independent from IFN-gamma sensitization, indicating that the apoptosis- and NF-kappaB-related FasL-IFN-gamma cross talk was not due to a simple global enhancement of Fas signaling. Overexpression of FLIP(L) and FLIP(S) inhibited Fas- as well as TRAIL-mediated NF-kappaB activation and apoptosis induction in IFN-gamma-primed cells suggesting that both responses are coregulated at the level of the DISC.

Published

2005

12. Membrane lymphotoxin-α2β is a novel tumor necrosis factor (TNF) receptor 2 (TNFR2) agonist

Author

Kucka, Kirstin, Lang, Isabell, Zhang, Tengyu, Siegmund, Daniela, Medler, Juliane, and Wajant, Harald

Subjects

Membranes, lcsh:Cytology, Receptors, Tumor Necrosis Factor, Type I, Tumor Necrosis Factor-alpha, Cytokines, Humans, Receptors, Tumor Necrosis Factor, Type II, ddc:610, lcsh:QH573-671, respiratory system, Signal transduction, Lymphotoxin-alpha, Article

Abstract

In the early 1990s, it has been described that LTα and LTβ form LTα\(_2\)β and LTαβ\(_2\) heterotrimers, which bind to TNFR1 and LTβR, respectively. Afterwards, the LTαβ\(_2\)–LTβR system has been intensively studied while the LTα\(_2\)β–TNFR1 interaction has been ignored to date, presumably due to the fact that at the time of identification of the LTα\(_2\)β–TNFR1 interaction one knew already two ligands for TNFR1, namely TNF and LTα. Here, we show that LTα\(_2\)β interacts not only with TNFR1 but also with TNFR2. We furthermore demonstrate that membrane-bound LTα\(_2\)β (memLTα\(_2\)β), despite its asymmetric structure, stimulates TNFR1 and TNFR2 signaling. Not surprising in view of its ability to interact with TNFR2, LTα\(_2\)β is inhibited by Etanercept, which is approved for the treatment of rheumatoid arthritis and also inhibits TNF and LTα.

Published

2021

13. TRAF2 Controls Death Receptor-Induced Caspase-8 Processing and Facilitates Proinflammatory Signaling

Author

Kreckel, Jennifer, Anany, Mohammed A., Siegmund, Daniela, and Wajant, Harald

Subjects

Immunology, Apoptosis, caspase-8, Cell Line, Cell Line, Tumor, death receptors, Humans, ddc:610, fas Receptor, TRAILR2, TRAILR1, Original Research, Inflammation, Caspase 8, Interleukin-8, NF-kappa B, Receptors, Death Domain, HCT116 Cells, TNF Receptor-Associated Factor 2, Up-Regulation, TNFR1, TRAF1, TRAF2, HEK293 Cells, Receptors, Tumor Necrosis Factor, Type I, CD95, Signal Transduction

Abstract

Tumor necrosis factor (TNF) receptor associated factor-2 (TRAF2) knockout (KO) cells were generated to investigate the role of TRAF2 in signaling by TNFR1 and the CD95-type death receptors (DRs) TRAILR1/2 and CD95. To prevent negative selection effects arising from the increased cell death sensitivity of TRAF2-deficient cells, cell lines were used for the generation of the TRAF2 KO variants that were protected from DR-induced apoptosis downstream of caspase-8 activation. As already described in the literature, TRAF2 KO cells displayed enhanced constitutive alternative NFκB signaling and reduced TNFR1-induced activation of the classical NFκB pathway. There was furthermore a significant but only partial reduction in CD95-type DR-induced upregulation of the proinflammatory NFκB-regulated cytokine interleukin-8 (IL8), which could be reversed by reexpression of TRAF2. In contrast, expression of the TRAF2-related TRAF1 protein failed to functionally restore TRAF2 deficiency. TRAF2 deficiency resulted furthermore in enhanced procaspase-8 processing by DRs, but this surprisingly came along with a reduction in net caspase-8 activity. In sum, our data argue for (i) a non-obligate promoting function of TRAF2 in proinflammatory DR signaling and (ii) a yet unrecognized stabilizing effect of TRAF2 on caspase-8 activity.

Published

2019