Your search keyword '"Vettorazzi S"' showing total 28 results

1. Inhibition of sphingosine 1-phosphate protects mice against chondrocyte catabolism and osteoarthritis

Author

Cherifi, C., Latourte, A., Vettorazzi, S., Tuckermann, J., Provot, S., Ea, H.-K., Ledoux, A., Casas, J., Cuvillier, O., Richette, P., Ostertag, A., Hay, E., and Cohen-Solal, M.

Published

2021

2. Blockage of sphingosin 1 phosphate S1P/S1PR pathway prevents from osteoarthritis in mice by reducing chondrocyte catabolism

Author

Cherifi, C., primary, Latourte, A., additional, Cuvillier, O., additional, Ea, K., additional, Vettorazzi, S., additional, Tuckermann, J., additional, Richette, P., additional, Hay, E., additional, and Cohen-Solal, M., additional

Published

2018

3. Deletion of Menin in craniofacial osteogenic cells in mice elicits development of mandibular ossifying fibroma

Author

Lee, S, primary, Liu, P, additional, Teinturier, R, additional, Jakob, J, additional, Tschaffon, M, additional, Tasdogan, A, additional, Wittig, R, additional, Hoeller, S, additional, Baumhoer, D, additional, Frappart, L, additional, Vettorazzi, S, additional, Bertolino, P, additional, Zhang, C, additional, and Tuckermann, J, additional

Published

2017

4. Deletion of Menin in craniofacial osteogenic cells in mice elicits development of mandibular ossifying fibroma

Author

Lee, S, Liu, P, Teinturier, R, Jakob, J, Tschaffon, M, Tasdogan, A, Wittig, R, Hoeller, S, Baumhoer, D, Frappart, L, Vettorazzi, S, Bertolino, P, Zhang, C, and Tuckermann, J

Abstract

Ossifying fibroma (OF) is a rare benign tumor of the craniofacial bones that can reach considerable and disfiguring dimensions if left untreated. Although the clinicopathological characteristics of OF are well established, the underlying etiology has remained largely unknown. Our work indicates that Men1—a tumor suppressor gene responsible of Multiple endocrine neoplasia type 1—is critical for OF formation and shows that mice with targeted disruption of Men1 in osteoblasts (Men1Runx2Cre) develop multifocal OF in the mandible with a 100% penetrance. Using lineage-tracing analysis, we demonstrate that loss of Men1 arrests stromal osteoprogenitors in OF at the osterix-positive pre-osteoblastic differentiation stage. Analysis of Men1-lacking stromal spindle cells isolated from OF (OF-derived MSCs (OFMSCs)) revealed a downregulation of the cyclin-dependent kinase (CDK) inhibitor Cdkn1a, consistent with an increased proliferation rate. Intriguingly, the re-expression of Men1 in Men1-deficient OFMSCs restored Cdkn1a expression and abrogated cellular proliferation supporting the tumor-suppressive role of Men1 in OF. Although our work presents the first evidence of Men1 in OF development, it further provides the first genetic mouse model of OF that can be used to better understand the molecular pathogenesis of these benign tumors and to potentially develop novel treatment strategies.

Published

2018

5. Acetylation-induced proteasomal degradation of the activated glucocorticoid receptor limits hormonal signaling.

Author

Iyer-Bierhoff A, Wieczorek M, Peter SM, Ward D, Bens M, Vettorazzi S, Guehrs KH, Tuckermann JP, and Heinzel T

Abstract

Glucocorticoid (GC) signaling is essential for mounting a stress response, however, chronic stress or prolonged GC therapy downregulates the GC receptor (GR), leading to GC resistance. Regulatory mechanisms that refine this equilibrium are not well understood. Here, we identify seven lysine acetylation sites in the amino terminal domain of GR, with lysine 154 (Lys 154 ) in the AF-1 region being the dominant acetyl-acceptor. GR-Lys 154 acetylation is mediated by p300/CBP in the nucleus in an agonist-dependent manner and correlates with transcriptional activity. Deacetylation by NAD + -dependent SIRT1 facilitates dynamic regulation of this mark. Notably, agonist-binding to both wild-type GR and an acetylation-deficient mutant elicits similar short-term target gene expression. In contrast, upon extended treatment, the polyubiquitination of the acetylation-deficient GR mutant is impaired resulting in higher protein stability, increased chromatin association and prolonged transactivation. Taken together, reversible acetylation fine-tunes duration of the GC response by regulating proteasomal degradation of activated GR., Competing Interests: Authors declare that they have no competing interests., (© 2024 The Author(s).)

Published

2024

6. Intact GR dimerization is critical for restraining plasma ACTH levels during chronic psychosocial stress.

Author

Langgartner D, Koenen M, Kupfer S, Glogger L, Kurz L, Perez-Rivas LG, Theodoropoulou M, Noll-Hussong M, Vettorazzi S, Tuckermann J, and Reber SO

Abstract

Male C57BL/6N mice exposed to the chronic subordinate colony housing (CSC; 19 days) paradigm, a preclinically validated model of chronic psychosocial stress, are characterized by unaffected basal morning plasma corticosterone (CORT) concentrations despite adrenal and pituitary hyperplasia and increased adrenocorticotropic hormone (ACTH) plasma concentrations, compared with single-housed control (SHC) mice. However, as CSC mice are still able to show an increased CORT secretion towards novel heterotypic stressors, these effects might reflect an adaptation rather than a functional breakdown of general hypothalamus-pituitary-adrenal (HPA) axis functionality. In the present study we used male mice of a genetically modified mouse line, to investigate whether genetically-driven ACTH overexpression compromises adaptational processes occurring at the level of the adrenals during CSC exposure. Experimental mice carried a point mutation in the DNA binding domain of the glucocorticoid (GC) receptor (GR), attenuating dimerization of GR (GR dim ), resulting in a congenially compromised negative feedback inhibition at the level of the pituitary. In line with previous studies, CSC mice in both the wild type (WT; GR +/+ ) and GR dim group developed adrenal enlargement. Moreover, compared with respective SHC and WT mice, CSC GR dim mice show increased basal morning plasma ACTH and CORT concentrations. Quantitative polymerase chain reaction (qPCR) analysis revealed neither a genotype effect, nor a CSC effect on pituitary mRNA expression of the ACTH precursor proopiomelanocortin (POMC). Finally, CSC increased anxiety-related behavior, active coping and splenocyte in vitro (re)activity in both WT and GR dim mice, while a CSC-induced increase in adrenal lipid vesicles and splenic GC resistance was detectable only in WT mice. Of note, lipopolysaccharide (LPS)-stimulated splenocytes of GR dim mice were resistant to the inhibitory effects of CORT. Together our findings support the hypothesis that pituitary ACTH protein concentration is negatively controlled by GR dimerization under conditions of chronic psychosocial stress, while POMC gene transcription is not dependent on intact GR dimerization under both basal and chronic stress conditions. Finally, our data suggest that adrenal adaptations during chronic psychosocial stress (i.e., ACTH desensitization), aiming at the prevention of prolonged hypercorticism, are protective only to a certain threshold of plasma ACTH levels., Competing Interests: DL, MK, SK, LG, LK, MT, MNH, SV, JT and SOR have nothing to declare and do not have any conflict of interest., (© 2023 The Authors.)

Published

2023

7. A guide to changing paradigms of glucocorticoid receptor function-a model system for genome regulation and physiology.

Author

Vettorazzi S, Nalbantoglu D, Gebhardt JCM, and Tuckermann J

Subjects

Animals, DNA, Ligands, Mice, Rats, Receptors, Cytoplasmic and Nuclear, Transcription Factors genetics, Zebrafish genetics, Glucocorticoids metabolism, Glucocorticoids pharmacology, Receptors, Glucocorticoid genetics, Receptors, Glucocorticoid metabolism

Abstract

The glucocorticoid receptor (GR) is a bona fide ligand-regulated transcription factor. Cloned in the 80s, the GR has become one of the best-studied and clinically most relevant members of the nuclear receptor superfamily. Cooperative activity of GR with other transcription factors and a plethora of coregulators contribute to the tissue- and context-specific response toward the endogenous and pharmacological glucocorticoids (GCs). Furthermore, nontranscriptional activities in the cytoplasm are emerging as an additional function of GR. Over the past 40 years, the concepts of GR mechanisms of action had been constantly changing. Different methodologies in the pregenomic and genomic era of molecular biological research and recent cutting-edge technology in single-cell and single-molecule analysis are steadily evolving the views, how the GR in particular and transcriptional regulation in general act in physiological and pathological processes. In addition to the development of technologies for GR analysis, the use of model organisms provides insights how the GR in vivo executes GC action in tissue homeostasis, inflammation, and energy metabolism. The model organisms, namely the mouse, but also rats, zebrafish, and recently fruit flies carrying mutations of the GR became a major driving force to analyze the molecular function of GR in disease models. This guide provides an overview of the exciting research and paradigm shifts in the GR field from past to present with a focus on GR transcription factor networks, GR DNA-binding and single-cell analysis, and model systems., (© 2021 The Authors. The FEBS Journal published by John Wiley & Sons Ltd on behalf of Federation of European Biochemical Societies.)

Published

2022

8. Cigarette smoke exposure reduces hemorrhagic shock induced circulatory dysfunction in mice with attenuated glucocorticoid receptor function.

Author

Wepler M, Preuss JM, Tilp C, Keck M, Blender J, Wachter U, Merz T, Vogt J, Kress S, Gröger M, Hoffmann A, Fink M, Calzia E, Burret U, Radermacher P, Tuckermann JP, and Vettorazzi S

Subjects

Animals, Catecholamines, Corticosterone, Cytokines metabolism, Glucocorticoids, Hypoxia complications, Lactates, Mice, Norepinephrine, Receptors, Glucocorticoid genetics, Receptors, Glucocorticoid metabolism, Cigarette Smoking, Lung Diseases complications, Pulmonary Disease, Chronic Obstructive metabolism, Shock, Hemorrhagic complications

Abstract

Introduction: We previously showed that attenuated glucocorticoid receptor (GR) function in mice (GR dim/dim ) aggravates systemic hypotension and impairs organ function during endotoxic shock. Hemorrhagic shock (HS) causes impaired organ perfusion, which leads to tissue hypoxia and inflammation with risk of organ failure. Lung co-morbidities like chronic obstructive pulmonary disease (COPD) can aggravate tissue hypoxia via alveolar hypoxia. The most common cause for COPD is cigarette smoke (CS) exposure. Therefore, we hypothesized that affecting GR function in mice (GR dim/dim ) and pre-traumatic CS exposure would further impair hemodynamic stability and organ function after HS., Methods: After 3 weeks of CS exposure, anesthetized and mechanically ventilated GR dim/dim and GR +/+ mice underwent pressure-controlled HS for 1h via blood withdrawal (mean arterial pressure (MAP) 35mmHg), followed by 4h of resuscitation with re-transfusion of shed blood, colloid fluid infusion and, if necessary, continuous intravenous norepinephrine. Acid-base status and organ function were assessed together with metabolic pathways. Blood and organs were collected at the end of the experiment for analysis of cytokines, corticosterone level, and mitochondrial respiratory capacity. Data is presented as median and interquartile range., Results: Nor CS exposure neither attenuated GR function affected survival. Non-CS GR dim/dim mice had a higher need of norepinephrine to keep target hemodynamics compared to GR +/+ mice. In contrast, after CS exposure norepinephrine need did not differ significantly between GR dim/dim and GR +/+ mice. Non-CS GR dim/dim mice presented with a lower pH and increased blood lactate levels compared to GR +/+ mice, but not CS exposed mice. Also, higher plasma concentrations of some pro-inflammatory cytokines were observed in non-CS GR dim/dim compared to GR +/+ mice, but not in the CS group. With regards to metabolic measurements, CS exposure led to an increased lipolysis in GR dim/dim compared to GR +/+ mice, but not in non-CS exposed animals., Conclusion: Whether less metabolic acidosis or increased lipolysis is the reason or the consequence for the trend towards lower catecholamine need in CS exposed GR dim/dim mice warrants further investigation., Competing Interests: Authors CT, MK, and JB are employed by Boehringer Ingelheim Pharma GmbH & Co KG. The remaining authors declare that the research was conducted in the absence of any commercial or financial relationships that could be construed as a potential conflict of interest., (Copyright © 2022 Wepler, Preuss, Tilp, Keck, Blender, Wachter, Merz, Vogt, Kress, Gröger, Hoffmann, Fink, Calzia, Burret, Radermacher, Tuckermann and Vettorazzi.)

Published

2022

9. Inhibition of Cdk5 increases osteoblast differentiation and bone mass and improves fracture healing.

Author

Ahmad M, Krüger BT, Kroll T, Vettorazzi S, Dorn AK, Mengele F, Lee S, Nandi S, Yilmaz D, Stolz M, Tangudu NK, Vázquez DC, Pachmayr J, Cirstea IC, Spasic MV, Ploubidou A, Ignatius A, and Tuckermann J

Abstract

Identification of regulators of osteoblastogenesis that can be pharmacologically targeted is a major goal in combating osteoporosis, a common disease of the elderly population. Here, unbiased kinome RNAi screening in primary murine osteoblasts identified cyclin-dependent kinase 5 (Cdk5) as a suppressor of osteoblast differentiation in both murine and human preosteoblastic cells. Cdk5 knockdown by siRNA, genetic deletion using the Cre-loxP system, or inhibition with the small molecule roscovitine enhanced osteoblastogenesis in vitro. Roscovitine treatment significantly enhanced bone mass by increasing osteoblastogenesis and improved fracture healing in mice. Mechanistically, downregulation of Cdk5 expression increased Erk phosphorylation, resulting in enhanced osteoblast-specific gene expression. Notably, simultaneous Cdk5 and Erk depletion abrogated the osteoblastogenesis conferred by Cdk5 depletion alone, suggesting that Cdk5 regulates osteoblast differentiation through MAPK pathway modulation. We conclude that Cdk5 is a potential therapeutic target to treat osteoporosis and improve fracture healing., (© 2022. The Author(s).)

Published

2022

10. Motoneuron-Specific PTEN Deletion in Mice Induces Neuronal Hypertrophy and Also Regeneration after Facial Nerve Injury.

Author

Meyer Zu Reckendorf S, Moser D, Blechschmidt A, Joga VN, Sinske D, Hegler J, Deininger S, Catanese A, Vettorazzi S, Antoniadis G, Boeckers T, and Knöll B

Subjects

Animals, Axons physiology, Female, Hyperplasia pathology, Hypertrophy pathology, Male, Mice, Motor Neurons metabolism, Tumor Suppressor Protein p53, Facial Nerve Injuries genetics, Facial Nerve Injuries pathology, Nerve Regeneration genetics, PTEN Phosphohydrolase metabolism

Abstract

In postmitotic neurons, several tumor suppressor genes (TSGs), including p53, Rb, and PTEN, modulate the axon regeneration success after injury. Particularly, PTEN inhibition is a key driver of successful CNS axon regeneration after optic nerve or spinal cord injury. In contrast, in peripheral neurons, TSG influence in neuronal morphology, physiology, and pathology has not been investigated to the same depth. In this study, we conditionally deleted PTEN from mouse facial motoneurons ( Chat-Cre/Pten loxP/loxP ) and analyzed neuronal responses in vivo with or without peripheral facial nerve injury in male and female mice. In uninjured motoneurons, PTEN loss induced somatic, axonal, and nerve hypertrophy, synaptic terminal enlargement and reduction in physiological whisker movement. Despite these morphologic and physiological changes, PTEN deletion positively regulated facial nerve regeneration and recovery of whisker movement after nerve injury. Regenerating PTEN-deficient motoneurons upregulated P-CREB and a signaling pathway involving P-Akt, P-PRAS40, P-mTOR, and P-4EBP1. In aged mice (12 months), PTEN deletion induced hair loss and facial hyperplasia of the epidermis. This suggests a time window in younger mice with PTEN loss stimulating axon growth after injury, however, at the risk of hyperplasia formation at later time points in the old animal. Overall, our data highlight a dual TSG function with PTEN loss impairing physiological neuron function but furthermore underscoring the positive effects of PTEN ablation in axon regeneration also for the PNS. SIGNIFICANCE STATEMENT Tumor suppressor genes (TSGs) restrict cell proliferation and growth. TSG inhibition, including p53 and PTEN, stimulates axon regeneration after CNS injury. In contrast, in PNS axon regeneration, TSGs have not been analyzed in great depth. Herein we show enhanced peripheral axon regeneration after PTEN deletion from facial motoneurons. This invokes a signaling cascade with novel PTEN partners, including CREB and PRAS40. In adult mice, PTEN loss induces hyperplasia of the skin epidermis, suggesting detrimental consequences when reaching adulthood in contrast to a beneficial TSG role for regeneration in young adult mice. Thus, our data highlight the double-edged sword nature of interfering with TSG function., (Copyright © 2022 the authors.)

Published

2022

11. Glucocorticoids coordinate macrophage metabolism through the regulation of the tricarboxylic acid cycle.

Author

Stifel U, Wolfschmitt EM, Vogt J, Wachter U, Vettorazzi S, Tews D, Hogg M, Zink F, Koll NM, Winning S, Mounier R, Chazaud B, Radermacher P, Fischer-Posovszky P, Caratti G, and Tuckermann J

Subjects

Humans, Inflammation metabolism, Macrophages metabolism, Receptors, Glucocorticoid genetics, Receptors, Glucocorticoid metabolism, Citric Acid Cycle, Glucocorticoids pharmacology

Abstract

Objectives: Glucocorticoids (GCs) are one of the most widely prescribed anti-inflammatory drugs. By acting through their cognate receptor, the glucocorticoid receptor (GR), GCs downregulate the expression of pro-inflammatory genes and upregulate the expression of anti-inflammatory genes. Metabolic pathways have recently been identified as key parts of both the inflammatory activation and anti-inflammatory polarization of macrophages, immune cells responsible for acute inflammation and tissue repair. It is currently unknown whether GCs control macrophage metabolism, and if so, to what extent metabolic regulation by GCs confers anti-inflammatory activity., Methods: Using transcriptomic and metabolomic profiling of macrophages, we identified GC-controlled pathways involved in metabolism, especially in mitochondrial function., Results: Metabolic analyses revealed that GCs repress glycolysis in inflammatory myeloid cells and promote tricarboxylic acid (TCA) cycle flux, promoting succinate metabolism and preventing intracellular accumulation of succinate. Inhibition of ATP synthase attenuated GC-induced transcriptional changes, likely through stalling of TCA cycle anaplerosis. We further identified a glycolytic regulatory transcription factor, HIF1α, as regulated by GCs, and as a key regulator of GC responsiveness during inflammatory challenge., Conclusions: Our findings link metabolism to gene regulation by GCs in macrophages., (Copyright © 2021 The Author(s). Published by Elsevier GmbH.. All rights reserved.)

Published

2022

12. Inhibition of Cdk5 Ameliorates Skeletal Bone Loss in Glucocorticoid-Treated Mice.

Author

Krüger BT, Steppe L, Vettorazzi S, Haffner-Luntzer M, Lee S, Dorn AK, Ignatius A, Tuckermann J, and Ahmad M

Abstract

Glucocorticoids (GCs) are widely used to treat inflammatory diseases. However, their long-term use leads to glucocorticoid-induced osteoporosis, increasing morbidity and mortality. Both anabolic and anti-resorptive drugs are used to counteract GC-induced bone loss, however, they are expensive and/or have major side effects. Therefore, identifying new targets for cost-effective, small-molecule inhibitors is essential. We recently identified cyclin-dependent kinase 5 (Cdk5) as a suppressor of osteoblast differentiation and showed that its inhibition with roscovitine promoted osteoblastogenesis, thus improving the skeletal bone mass and fracture healing. Here, we assessed whether Cdk5 knockdown or inhibition could also reverse the GC-mediated suppression of osteoblast differentiation, bone loss, and fracture healing. We first demonstrated that Cdk5 silencing abolished the dexamethasone (Dex)-induced downregulation of alkaline phosphatase (Alp) activity, osteoblast-specific marker gene expression ( Runx2 , Sp7 , Alpl , and Bglap ), and mineralization. Similarly, Cdk5 inhibition rescued Dex-induced suppression of Alp activity. We further demonstrated that Cdk5 inhibition reversed prednisolone (Pred)-induced bone loss in mice, due to reduced osteoclastogenesis rather than improved osteoblastogenesis. Moreover, we revealed that Cdk5 inhibition failed to improve Pred-mediated impaired fracture healing. Taken together, we demonstrated that Cdk5 inhibition with roscovitine ameliorated GC-mediated bone loss but did not reverse GC-induced compromised fracture healing in mice.

Published

2022

13. Impaired Glucocorticoid Receptor Signaling Aggravates Lung Injury after Hemorrhagic Shock.

Author

Preuss JM, Burret U, Gröger M, Kress S, Scheuerle A, Möller P, Tuckermann JP, Wepler M, and Vettorazzi S

Subjects

Animals, Disease Models, Animal, Humans, Mice, Signal Transduction, Lung Injury therapy, Receptors, Glucocorticoid metabolism, Shock, Hemorrhagic complications

Abstract

We previously showed that attenuated lung injury after hemorrhagic shock (HS) coincided with enhanced levels of the glucocorticoid (GC) receptor (GR) in lung tissue of swine. Here, we investigated the effects of impaired GR signaling on the lung during resuscitated HS using a dysfunctional GR mouse model (GR dim/dim ). In a mouse intensive care unit, HS led to impaired lung mechanics and aggravated lung inflammation in GR dim/dim mice compared to wildtype mice (GR +/+ ). After HS, high levels of the pro-inflammatory and pro-apoptotic transcription factor STAT1/pSTAT1 were found in lung samples from GR dim/dim mice. Lungs of GR dim/dim mice revealed apoptosis, most likely as consequence of reduced expression of the lung-protective Angpt1 compared to GR +/+ after HS. RNA-sequencing revealed increased expression of pro-apoptotic and cytokine-signaling associated genes in lung tissue of GR dim/dim mice. Furthermore, high levels of pro-inflammatory cytokines and iNOS were found in lungs of GR dim/dim mice. Our results indicate impaired repression of STAT1/pSTAT1 due to dysfunctional GR signaling in GR dim/dim mice, which leads to increased inflammation and apoptosis in the lungs. These data highlight the crucial role of functional GR signaling to attenuate HS-induced lung damage.

Published

2021

14. The Role of Glucocorticoids in Inflammatory Diseases.

Author

Reichardt SD, Amouret A, Muzzi C, Vettorazzi S, Tuckermann JP, Lühder F, and Reichardt HM

Subjects

Animals, Disease Models, Animal, Humans, Inflammation pathology, Models, Biological, Nanoparticles chemistry, Phenotype, Glucocorticoids metabolism, Inflammation metabolism

Abstract

For more than 70 years, glucocorticoids (GCs) have been a powerful and affordable treatment option for inflammatory diseases. However, their benefits do not come without a cost, since GCs also cause side effects. Therefore, strong efforts are being made to improve their therapeutic index. In this review, we illustrate the mechanisms and target cells of GCs in the pathogenesis and treatment of some of the most frequent inflammatory disorders affecting the central nervous system, the gastrointestinal tract, the lung, and the joints, as well as graft-versus-host disease, which often develops after hematopoietic stem cell transplantation. In addition, an overview is provided of novel approaches aimed at improving GC therapy based on chemical modifications or GC delivery using nanoformulations. GCs remain a topic of highly active scientific research despite being one of the oldest class of drugs in medical use.

Published

2021

15. Deletion of Cdk5 in Macrophages Ameliorates Anti-Inflammatory Response during Endotoxemia through Induction of C-Maf and Il-10.

Author

Pfänder P, Eiers AK, Burret U, and Vettorazzi S

Subjects

Animals, Cells, Cultured, Chemokines genetics, Chemokines metabolism, Cyclin-Dependent Kinase 5 metabolism, Cytokines genetics, Cytokines metabolism, Endotoxemia chemically induced, Endotoxemia metabolism, Gene Expression Regulation, Inflammation metabolism, Interleukin-10 metabolism, Lipopolysaccharides, Lung metabolism, Lung pathology, Mice, Inbred C57BL, Mice, Knockout, Proto-Oncogene Proteins c-maf metabolism, Mice, Cyclin-Dependent Kinase 5 genetics, Endotoxemia genetics, Inflammation genetics, Interleukin-10 genetics, Macrophages metabolism, Proto-Oncogene Proteins c-maf genetics

Abstract

Immune response control is critical as excessive cytokine production can be detrimental and damage the host. Interleukin-10 (Il-10), an anti-inflammatory cytokine produced primarily by macrophages, is a key regulator that counteracts and controls excessive inflammatory response. Il-10 expression is regulated through the transcription factor c-Maf. Another regulator of Il-10 production is p35, an activator of the cyclin-dependent kinase 5 (Cdk5), which decreases Il-10 production in macrophages, thus increasing inflammation. However, Cdk5 regulation of c-Maf and the involvement of Il-10 production in macrophages has not yet been investigated. We used in vitro primary bone marrow-derived macrophages (BMDMs) lacking Cdk5 , stimulated them with lipopolysaccharid (LPS) and observed increased levels of c-Maf and Il-10. In an in vivo mouse model of LPS-induced endotoxemia, mice lacking Cdk5 in macrophages showed increased levels of c-Maf and elevated levels of Il-10 in lungs as well as in plasma, resulting in ameliorated survival. Taken together, we identified Cdk5 as a potential novel regulator of Il-10 production through c-Maf in macrophages under inflammatory conditions. Our results suggest that inhibition of Cdk5 enhances the c-Maf-Il-10 axis and thus potentiates improvement of anti-inflammatory therapy.

Published

2021

16. A physiological glucocorticoid rhythm is an important regulator of brown adipose tissue function.

Author

Kroon J, Schilperoort M, In Het Panhuis W, van den Berg R, van Doeselaar L, Verzijl CRC, van Trigt N, Mol IM, Sips HHCM, van den Heuvel JK, Koorneef LL, van der Sluis RJ, Fenzl A, Kiefer FW, Vettorazzi S, Tuckermann JP, Biermasz NR, Meijer OC, Rensen PCN, and Kooijman S

Subjects

Adipocytes metabolism, Adipocytes pathology, Adipose Tissue, Brown pathology, Adiposity, Animals, Corticosterone metabolism, Fatty Acids metabolism, Female, Lipid Metabolism physiology, Male, Mice, Mice, Inbred C57BL, Obesity metabolism, Period Circadian Proteins genetics, Period Circadian Proteins metabolism, Receptors, Glucocorticoid genetics, Transcriptome, Triglycerides metabolism, Adipose Tissue, Brown metabolism, Circadian Rhythm physiology, Glucocorticoids metabolism, Receptors, Glucocorticoid metabolism

Abstract

Objective: Brown adipose tissue (BAT) displays a strong circadian rhythm in metabolic activity, but it is unclear how this rhythm is regulated. As circulating levels of corticosterone coincide with the rhythm of triglyceride-derived fatty acid (FA) uptake by BAT, we investigated whether corticosterone regulates BAT circadian rhythm., Methods: Corticosterone levels were flattened by implanting mice with subcutaneous corticosterone-releasing pellets, resulting in constant circulating corticosterone levels., Results: Flattened corticosterone rhythm caused a complete loss of circadian rhythm in triglyceride-derived fatty acid uptake by BAT. This effect was independent of glucocorticoid receptor expression in (brown) adipocytes and was not caused by deregulation of clock gene expression or overexposure to glucocorticoids, but rather seemed mediated by reduced sympathetic innervation of BAT. In a mouse model of hyperlipidemia and metabolic syndrome, long-term experimental flattening of corticosterone - and thus rhythm in BAT function - resulted in adiposity., Conclusions: This study highlights that a physiological rhythm in glucocorticoids is an important regulator of BAT function and essential for the maintenance of metabolic health., (Copyright © 2021 The Author(s). Published by Elsevier GmbH.. All rights reserved.)

Published

2021

17. Impact of downstream effects of glucocorticoid receptor dysfunction on organ function in critical illness-associated systemic inflammation.

Author

Wepler M, Preuss JM, Merz T, McCook O, Radermacher P, Tuckermann JP, and Vettorazzi S

Abstract

Glucocorticoids (GCs) are stress hormones that regulate developmental and physiological processes and are among the most potent anti-inflammatory drugs to suppress chronic and acute inflammation. GCs act through the glucocorticoid receptor (GR), a ubiquitously expressed ligand-activated transcription factor, which translocates into the nucleus and can act via two different modes, as a GR monomer or as a GR dimer. These two modes of action are not clearly differentiated in practice and may lead to completely different therapeutic outcomes. Detailed aspects of GR mechanisms are often not taken into account when GCs are used in different clinical scenarios. Patients, with critical illness-related corticosteroid insufficiency, treated with natural or synthetic GCs are still missing a clearly defined therapeutic strategy. This review discusses the different modes of GR function and its importance on organ function in vivo.

Published

2020

18. The Role of Glucocorticoid Receptor and Oxytocin Receptor in the Septic Heart in a Clinically Relevant, Resuscitated Porcine Model With Underlying Atherosclerosis.

Author

Merz T, Denoix N, Wigger D, Waller C, Wepler M, Vettorazzi S, Tuckermann J, Radermacher P, and McCook O

Subjects

Animals, Cystathionine gamma-Lyase genetics, Disease Models, Animal, Heart Diseases etiology, Heart Diseases metabolism, Hydrogen Sulfide metabolism, Male, Oxidative Stress, Receptors, Glucocorticoid genetics, Receptors, Oxytocin genetics, Signal Transduction, Swine, Atherosclerosis physiopathology, Cystathionine gamma-Lyase metabolism, Gene Expression Regulation, Heart Diseases pathology, Hypercholesterolemia physiopathology, Receptors, Glucocorticoid metabolism, Receptors, Oxytocin metabolism, Shock, Septic complications

Abstract

The pathophysiology of sepsis-induced myocardial dysfunction is not resolved to date and comprises inflammation, barrier dysfunction and oxidative stress. Disease-associated reduction of tissue cystathionine-γ-lyase (CSE) expression, an endogenous H 2 S-producing enzyme, is associated with oxidative stress, barrier dysfunction and organ injury. CSE-mediated cardio-protection has been suggested to be related the upregulation of oxytocin receptor (OTR). CSE can also mediate glucocorticoid receptor (GR) signaling, which is important for normal heart function. A sepsis-related loss of cardiac CSE expression associated with impaired organ function has been reported previously. The aim of this current post hoc study was to investigate the role of cardiac GR and OTR after polymicrobial sepsis in a clinically relevant, resuscitated, atherosclerotic porcine model. Anesthetized and instrumented FBM (Familial Hypercholesterolemia Bretoncelles Meishan) pigs with high fat diet-induced atherosclerosis underwent poly-microbial septic shock ( n = 8) or sham procedure ( n = 5), and subsequently received intensive care therapy with fluid and noradrenaline administration for 24 h. Cardiac protein expression and mRNA levels were analyzed. Systemic troponin, a marker of cardiac injury, was significantly increased in septic animals in contrast to sham, whereas OTR and GR expression in septic hearts were reduced, along with a down-regulation of anti-inflammatory GR target genes and the antioxidant transcription factor NRF2. These results suggest a potential interplay between GR, CSE, and OTR in sepsis-mediated oxidative stress, inflammation and cardiac dysfunction., (Copyright © 2020 Merz, Denoix, Wigger, Waller, Wepler, Vettorazzi, Tuckermann, Radermacher and McCook.)

Published

2020

19. Impaired Glucocorticoid Receptor Dimerization Aggravates LPS-Induced Circulatory and Pulmonary Dysfunction.

Author

Wepler M, Preuss JM, Merz T, Hartmann C, Wachter U, McCook O, Vogt J, Kress S, Gröger M, Fink M, Scheuerle A, Möller P, Calzia E, Burret U, Radermacher P, Tuckermann JP, and Vettorazzi S

Subjects

Acute Lung Injury etiology, Acute Lung Injury metabolism, Animals, Dimerization, Mice, Protein Multimerization, Shock, Septic complications, Lipopolysaccharides toxicity, Receptors, Glucocorticoid chemistry, Receptors, Glucocorticoid metabolism, Shock, Septic metabolism, Shock, Septic physiopathology

Abstract

Background: Sepsis, that can be modeled by LPS injections, as an acute systemic inflammation syndrome is the most common cause for acute lung injury (ALI). ALI induces acute respiratory failure leading to hypoxemia, which is often associated with multiple organ failure (MOF). During systemic inflammation, the hypothalamus-pituitary-adrenal axis (HPA) is activated and anti-inflammatory acting glucocorticoids (GCs) are released to overcome the inflammation. GCs activate the GC receptor (GR), which mediates its effects via a GR monomer or GR dimer. The detailed molecular mechanism of the GR in different inflammatory models and target genes that might be crucial for resolving inflammation is not completely identified. We previously observed that mice with attenuated GR dimerization (GR dim/dim ) had a higher mortality in a non-resuscitated lipopolysaccharide (LPS)- and cecal ligation and puncture (CLP)-induced inflammation model and are refractory to exogenous GCs to ameliorate ALI during inflammation. Therefore, we hypothesized that impaired murine GR dimerization (GR dim/dim ) would further impair organ function in LPS-induced systemic inflammation under human like intensive care management and investigated genes that are crucial for lung function in this setup. Methods: Anesthetized GR dim/dim and wildtype (GR +/+ ) mice were challenged with LPS (10 mg·kg -1 , intraperitoneal) and underwent intensive care management ("lung-protective" mechanical ventilation, crystalloids, and norepinephrine) for 6 h. Lung mechanics and gas exchange were assessed together with systemic hemodynamics, acid-base status, and mitochondrial oxygen consumption (JO 2 ). Western blots, immunohistochemistry, and real time quantitative polymerase chain reaction were performed to analyze lung tissue and inflammatory mediators were analyzed in plasma and lung tissue. Results: When animals were challenged with LPS and subsequently resuscitated under intensive care treatment, GR dim/dim mice had a higher mortality compared to GR +/+ mice, induced by an increased need of norepinephrine to achieve hemodynamic targets. After challenge with LPS, GR dim/dim mice also displayed an aggravated ALI shown by a more pronounced impairment of gas exchange, lung mechanics and increased osteopontin (Opn) expression in lung tissue. Conclusion: Impairment of GR dimerization aggravates systemic hypotension and impairs lung function during LPS-induced endotoxic shock in mice. We demonstrate that the GR dimer is an important mediator of hemodynamic stability and lung function, possibly through regulation of Opn, during LPS-induced systemic inflammation., (Copyright © 2020 Wepler, Preuss, Merz, Hartmann, Wachter, McCook, Vogt, Kress, Gröger, Fink, Scheuerle, Möller, Calzia, Burret, Radermacher, Tuckermann and Vettorazzi.)

Published

2020

20. Fighting the Fire: Mechanisms of Inflammatory Gene Regulation by the Glucocorticoid Receptor.

Author

Escoter-Torres L, Caratti G, Mechtidou A, Tuckermann J, Uhlenhaut NH, and Vettorazzi S

Subjects

Animals, Glucocorticoids pharmacology, Humans, Immunosuppressive Agents pharmacology, Gene Expression Regulation drug effects, Gene Expression Regulation immunology, Glucocorticoids immunology, Immunosuppressive Agents immunology, Receptors, Glucocorticoid immunology

Abstract

For many decades, glucocorticoids have been widely used as the gold standard treatment for inflammatory conditions. Unfortunately, their clinical use is limited by severe adverse effects such as insulin resistance, cardiometabolic diseases, muscle and skin atrophies, osteoporosis, and depression. Glucocorticoids exert their effects by binding to the Glucocorticoid Receptor (GR), a ligand-activated transcription factor which both positively, and negatively regulates gene expression. Extensive research during the past several years has uncovered novel mechanisms by which the GR activates and represses its target genes. Genome-wide studies and mouse models have provided valuable insight into the molecular mechanisms of inflammatory gene regulation by GR. This review focusses on newly identified target genes and GR co-regulators that are important for its anti-inflammatory effects in innate immune cells, as well as mutations within the GR itself that shed light on its transcriptional activity. This research progress will hopefully serve as the basis for the development of safer immune suppressants with reduced side effect profiles.

Published

2019

21. Cdk5 Deletion Enhances the Anti-inflammatory Potential of GC-Mediated GR Activation During Inflammation.

Author

Pfänder P, Fidan M, Burret U, Lipinski L, and Vettorazzi S

Subjects

Animals, Anti-Inflammatory Agents metabolism, Arthritis, Rheumatoid therapy, Cells, Cultured, Glucocorticoids metabolism, Humans, Mice, Mice, Inbred C57BL, Mice, Knockout, Sepsis therapy, Arthritis, Rheumatoid metabolism, Cyclin-Dependent Kinase 5 genetics, Inflammation metabolism, Macrophages immunology, Receptors, Glucocorticoid metabolism, Sepsis metabolism, Sequence Deletion genetics

Abstract

The suppression of activated pro-inflammatory macrophages during immune response has a major impact on the outcome of many inflammatory diseases including sepsis and rheumatoid arthritis. The pro- and anti-inflammatory functions of macrophages have been widely studied, whereas their regulation under immunosuppressive treatments such as glucocorticoid (GC) therapy is less well-understood. GC-mediated glucocorticoid receptor (GR) activation is crucial to mediate anti-inflammatory effects. In addition, the anti-cancer drug roscovitine, that is currently being tested in clinical trials, was recently described to regulate inflammatory processes by inhibiting different Cdks such as cyclin-dependent kinase 5 ( Cdk5 ). Cdk5 was identified as a modulator of inflammatory processes in different immune cells and furthermore described to influence GR gene expression in the brain. Whether roscovitine can enhance the immunosuppressive effects of GCs and if the inhibition of Cdk5 affects GR gene regulatory function in innate immune cells, such as macrophages, has not yet been investigated. Here, we report that roscovitine enhances the immunosuppressive Dexamethasone (Dex) effect on the inducible nitric oxide synthase (iNos) expression, which is essential for immune regulation. Cdk5 deletion in macrophages prevented iNos protein and nitric oxide (NO) generation after a combinatory treatment with inflammatory stimuli and Dex. Cdk5 deletion in macrophages attenuated the GR phosphorylation on serine 211 after Dex treatment alone and in combination with inflammatory stimuli, but interestingly increased the GR-dependent anti-inflammatory target gene dual-specificity phosphatase 1 (Dusp1, Mkp1). Mkp1 phosphatase activity decreases the activation of its direct target p38Mapk, reduced iNos expression and NO production upon inflammatory stimuli and Dex treatment in the absence of Cdk5 . Taken together, we identified Cdk5 as a potential novel regulator of NO generation in inflammatory macrophages under GC treatment. Our data suggest that GC treatment in combination with specific Cdk5 inhibtior(s) provides a stronger suppression of inflammation and could thus replace high-dose GC therapy which has severe side effects in the treatment of inflammatory diseases.

Published

2019

22. Insulin signaling and reduced glucocorticoid receptor activity attenuate postprandial gene expression in liver.

Author

Kalvisa A, Siersbæk MS, Præstholm SM, Christensen LJL, Nielsen R, Stohr O, Vettorazzi S, Tuckermann J, White M, Mandrup S, and Grøntved L

Subjects

Animals, Forkhead Transcription Factors metabolism, Gene Expression, Gene Expression Regulation genetics, Gene Expression Regulation physiology, Hepatocytes metabolism, Insulin genetics, Insulin Resistance, Liver metabolism, Male, Mice, Mice, Inbred C57BL, Obesity metabolism, Receptors, Glucocorticoid genetics, Signal Transduction drug effects, Insulin metabolism, Postprandial Period genetics, Receptors, Glucocorticoid metabolism

Abstract

Hepatic circadian gene transcription is tightly coupled to feeding behavior, which has a profound impact on metabolic disorders associated with diet-induced obesity. Here, we describe a genomics approach to uncover mechanisms controlling hepatic postprandial gene expression. Combined transcriptomic and cistromic analysis identified hundreds of circadian-regulated genes and enhancers controlled by feeding. Postprandial suppression of enhancer activity was associated with reduced glucocorticoid receptor (GR) and Forkhead box O1 (FOXO1) occupancy of chromatin correlating with reduced serum corticosterone levels and increased serum insulin levels. Despite substantial co-occupancy of feeding-regulated enhancers by GR and FOXO1, selective disruption of corticosteroid and/or insulin signaling resulted in dysregulation of specific postprandial regulated gene programs. In combination, these signaling pathways operate a major part of the genes suppressed by feeding. Importantly, the feeding response was disrupted in diet-induced obese animals, which was associated with dysregulation of several corticosteroid- and insulin-regulated genes, providing mechanistic insights to dysregulated circadian gene transcription associated with obesity., Competing Interests: The authors have declared that no competing interests exist.

Published

2018

23. Thirty-eight-negative kinase 1 mediates trauma-induced intestinal injury and multi-organ failure.

Author

Armacki M, Trugenberger AK, Ellwanger AK, Eiseler T, Schwerdt C, Bettac L, Langgartner D, Azoitei N, Halbgebauer R, Groß R, Barth T, Lechel A, Walter BM, Kraus JM, Wiegreffe C, Grimm J, Scheffold A, Schneider MR, Peuker K, Zeißig S, Britsch S, Rose-John S, Vettorazzi S, Wolf E, Tannapfel A, Steinestel K, Reber SO, Walther P, Kestler HA, Radermacher P, Barth TF, Huber-Lang M, Kleger A, and Seufferlein T

Subjects

Animals, Disease Models, Animal, Female, Fetal Proteins genetics, Inflammatory Bowel Diseases etiology, Inflammatory Bowel Diseases genetics, Inflammatory Bowel Diseases pathology, Interleukin-6 genetics, Interleukin-6 metabolism, Intestines pathology, Mice, Multiple Organ Failure etiology, Multiple Organ Failure genetics, Multiple Organ Failure pathology, Multiple Trauma complications, Multiple Trauma genetics, Multiple Trauma pathology, Protein-Tyrosine Kinases genetics, STAT3 Transcription Factor genetics, STAT3 Transcription Factor metabolism, Swine, Systemic Inflammatory Response Syndrome etiology, Systemic Inflammatory Response Syndrome pathology, Transcription Factor RelA genetics, Transcription Factor RelA metabolism, Tumor Necrosis Factor-alpha genetics, Tumor Necrosis Factor-alpha metabolism, Fetal Proteins metabolism, Inflammatory Bowel Diseases enzymology, Intestines enzymology, Multiple Organ Failure enzymology, Multiple Trauma enzymology, Protein-Tyrosine Kinases metabolism, Systemic Inflammatory Response Syndrome enzymology

Abstract

Dysregulated intestinal epithelial apoptosis initiates gut injury, alters the intestinal barrier, and can facilitate bacterial translocation leading to a systemic inflammatory response syndrome (SIRS) and/or multi-organ dysfunction syndrome (MODS). A variety of gastrointestinal disorders, including inflammatory bowel disease, have been linked to intestinal apoptosis. Similarly, intestinal hyperpermeability and gut failure occur in critically ill patients, putting the gut at the center of SIRS pathology. Regulation of apoptosis and immune-modulatory functions have been ascribed to Thirty-eight-negative kinase 1 (TNK1), whose activity is regulated merely by expression. We investigated the effect of TNK1 on intestinal integrity and its role in MODS. TNK1 expression induced crypt-specific apoptosis, leading to bacterial translocation, subsequent septic shock, and early death. Mechanistically, TNK1 expression in vivo resulted in STAT3 phosphorylation, nuclear translocation of p65, and release of IL-6 and TNF-α. A TNF-α neutralizing antibody partially blocked development of intestinal damage. Conversely, gut-specific deletion of TNK1 protected the intestinal mucosa from experimental colitis and prevented cytokine release in the gut. Finally, TNK1 was found to be deregulated in the gut in murine and porcine trauma models and human inflammatory bowel disease. Thus, TNK1 might be a target during MODS to prevent damage in several organs, notably the gut.

Published

2018

24. Erratum. Adipocyte Glucocorticoid Receptor Deficiency Attenuates Aging- and HFD-Induced Obesity and Impairs the Feeding-Fasting Transition. Diabetes 2017;66:272-286.

Author

Mueller KM, Hartmann K, Kaltenecker D, Vettorazzi S, Bauer M, Mauser L, Amann S, Jall S, Fischer K, Esterbauer H, Müller TD, Tschöp MH, Magnes C, Haybaeck J, Scherer T, Bordag N, Tuckermann JP, and Moriggl R

Published

2018

25. Molecular Integration of Incretin and Glucocorticoid Action Reverses Immunometabolic Dysfunction and Obesity.

Author

Quarta C, Clemmensen C, Zhu Z, Yang B, Joseph SS, Lutter D, Yi CX, Graf E, García-Cáceres C, Legutko B, Fischer K, Brommage R, Zizzari P, Franklin BS, Krueger M, Koch M, Vettorazzi S, Li P, Hofmann SM, Bakhti M, Bastidas-Ponce A, Lickert H, Strom TM, Gailus-Durner V, Bechmann I, Perez-Tilve D, Tuckermann J, Hrabě de Angelis M, Sandoval D, Cota D, Latz E, Seeley RJ, Müller TD, DiMarchi RD, Finan B, and Tschöp MH

Subjects

Animals, Body Weight drug effects, Dexamethasone analogs & derivatives, Energy Metabolism drug effects, Glucagon-Like Peptide 1 analogs & derivatives, Glucocorticoids chemistry, Glucose metabolism, HEK293 Cells, Humans, Hypothalamus drug effects, Hypothalamus metabolism, Incretins chemistry, Inflammation complications, Inflammation metabolism, Male, Mice, Mice, Inbred C57BL, Mice, Obese, Obesity complications, Obesity metabolism, Dexamethasone therapeutic use, Glucagon-Like Peptide 1 therapeutic use, Glucocorticoids therapeutic use, Incretins therapeutic use, Inflammation drug therapy, Obesity drug therapy

Abstract

Chronic inflammation has been proposed to contribute to the pathogenesis of diet-induced obesity. However, scarce therapeutic options are available to treat obesity and the associated immunometabolic complications. Glucocorticoids are routinely employed for the management of inflammatory diseases, but their pleiotropic nature leads to detrimental metabolic side effects. We developed a glucagon-like peptide-1 (GLP-1)-dexamethasone co-agonist in which GLP-1 selectively delivers dexamethasone to GLP-1 receptor-expressing cells. GLP-1-dexamethasone lowers body weight up to 25% in obese mice by targeting the hypothalamic control of feeding and by increasing energy expenditure. This strategy reverses hypothalamic and systemic inflammation while improving glucose tolerance and insulin sensitivity. The selective preference for GLP-1 receptor bypasses deleterious effects of dexamethasone on glucose handling, bone integrity, and hypothalamus-pituitary-adrenal axis activity. Thus, GLP-1-directed glucocorticoid pharmacology represents a safe and efficacious therapy option for diet-induced immunometabolic derangements and the resulting obesity., (Copyright © 2017 Elsevier Inc. All rights reserved.)

Published

2017

26. Adipocyte Glucocorticoid Receptor Deficiency Attenuates Aging- and HFD-Induced Obesity and Impairs the Feeding-Fasting Transition.

Author

Mueller KM, Hartmann K, Kaltenecker D, Vettorazzi S, Bauer M, Mauser L, Amann S, Jall S, Fischer K, Esterbauer H, Müller TD, Tschöp MH, Magnes C, Haybaeck J, Scherer T, Bordag N, Tuckermann JP, and Moriggl R

Subjects

Adenylyl Cyclases metabolism, Adipose Tissue metabolism, Adiposity genetics, Aging metabolism, Animals, Blotting, Western, Chromatography, Liquid, Diet, High-Fat, Energy Metabolism, Fatty Liver genetics, Hypertrophy, Insulin metabolism, Lipolysis, Mass Spectrometry, Metabolomics, Mice, Obesity metabolism, Receptors, Adrenergic, beta metabolism, Signal Transduction, Adipocytes metabolism, Aging genetics, Fasting, Feeding Behavior, Lipid Metabolism genetics, Liver metabolism, Obesity genetics, Receptors, Glucocorticoid genetics

Abstract

Glucocorticoids (GCs) are important regulators of systemic energy metabolism, and aberrant GC action is linked to metabolic dysfunctions. Yet, the extent to which normal and pathophysiological energy metabolism depend on the GC receptor (GR) in adipocytes remains unclear. Here, we demonstrate that adipocyte GR deficiency in mice significantly impacts systemic metabolism in different energetic states. Plasma metabolomics and biochemical analyses revealed a marked global effect of GR deficiency on systemic metabolite abundance and, thus, substrate partitioning in fed and fasted states. This correlated with a decreased lipolytic capacity of GR-deficient adipocytes under postabsorptive and fasting conditions, resulting from impaired signal transduction from β-adrenergic receptors to adenylate cyclase. Upon prolonged fasting, the impaired lipolytic response resulted in abnormal substrate utilization and lean mass wasting. Conversely, GR deficiency attenuated aging-/diet-associated obesity, adipocyte hypertrophy, and liver steatosis. Systemic glucose tolerance was improved in obese GR-deficient mice, which was associated with increased insulin signaling in muscle and adipose tissue. We conclude that the GR in adipocytes exerts central but diverging roles in the regulation of metabolic homeostasis depending on the energetic state. The adipocyte GR is indispensable for the feeding-fasting transition but also promotes adiposity and associated metabolic disorders in fat-fed and aged mice., (© 2017 by the American Diabetes Association.)

Published

2017

27. GR-independent down-modulation on GM-CSF bone marrow-derived dendritic cells by the selective glucocorticoid receptor modulator Compound A.

Author

Barcala Tabarrozzi AE, Andreone L, Deckers J, Castro CN, Gimeno ML, Ariolfo L, Berguer PM, Antunica-Noguerol M, Liberman AC, Vettorazzi S, Tuckermann JP, De Bosscher K, and Perone MJ

Subjects

Animals, B7-1 Antigen metabolism, Bone Marrow Cells cytology, Dendritic Cells cytology, Endocytosis drug effects, Inflammation Mediators antagonists & inhibitors, Lipopolysaccharides pharmacology, Mice, Toll-Like Receptor 4 drug effects, Toll-Like Receptor 4 metabolism, Tyramine pharmacology, Up-Regulation drug effects, Acetates pharmacology, Bone Marrow Cells drug effects, Dendritic Cells drug effects, Down-Regulation, Granulocyte-Macrophage Colony-Stimulating Factor physiology, Receptors, Glucocorticoid drug effects, Receptors, Glucocorticoid metabolism, Tyramine analogs & derivatives

Abstract

Dendritic cells (DC) initiate the adaptive immune response. Glucocorticoids (GCs) down-modulate the function of DC. Compound A (CpdA, (2-(4-acetoxyphenyl)-2-chloro-N-methyl-ethylammonium chloride) is a plant-derived GR-ligand with marked dissociative properties. We investigated the effects of CpdA on in vitro generated GM-CSF-conditioned bone marrow-derived DC (BMDC). CpdA-exposed BMDC exhibited low expression of cell-surface molecules and diminution of the release of proinflammatory cytokines upon LPS stimulation; processes associated with BMDC maturation and activation. CpdA-treated BMDC were inefficient at Ag capture via mannose receptor-mediated endocytosis and displayed reduced T-cell priming. CpdA prevented the LPS-induced rise in pErk1/2 and pP38, kinases involved in TLR4 signaling. CpdA fully inhibited LPS-induced pAkt Ser473 , a marker associated with the generation of tolerogenic DC. We used pharmacological blockade and selective genetic loss-of-function tools and demonstrated GR-independent inhibitory effects of CpdA in BMDC. Mechanistically, CpdA-mediated inactivation of the NF-κB intracellular signaling pathway was associated with a short-circuiting of pErk1/2 and pP38 upstream signaling. Assessment of the in vivo function of CpdA-treated BMDC pulsed with the hapten trinitrobenzenesulfonic acid showed impaired cell-mediated contact hypersensitivity. Collectively, we provide evidence that CpdA is an effective BMDC modulator that might have a benefit for immune disorders, even when GR is not directly targeted.

Published

2016

28. Glucocorticoids limit acute lung inflammation in concert with inflammatory stimuli by induction of SphK1.

Author

Vettorazzi S, Bode C, Dejager L, Frappart L, Shelest E, Klaßen C, Tasdogan A, Reichardt HM, Libert C, Schneider M, Weih F, Henriette Uhlenhaut N, David JP, Gräler M, Kleiman A, and Tuckermann JP

Subjects

Animals, Chromatin Immunoprecipitation, Cytokines drug effects, Cytokines immunology, Flow Cytometry, Gene Expression Regulation drug effects, Inflammation, Lysophospholipids metabolism, Macrophages immunology, Macrophages metabolism, Mice, Phosphotransferases (Alcohol Group Acceptor) genetics, Real-Time Polymerase Chain Reaction, Ribosomal Protein S6 Kinases, 90-kDa immunology, Sphingosine analogs & derivatives, Sphingosine metabolism, Transcriptional Activation drug effects, Up-Regulation, p38 Mitogen-Activated Protein Kinases immunology, Acute Lung Injury immunology, Glucocorticoids pharmacology, Macrophages drug effects, Phosphotransferases (Alcohol Group Acceptor) drug effects, Receptors, Glucocorticoid agonists

Abstract

Acute lung injury (ALI) is a severe inflammatory disease for which no specific treatment exists. As glucocorticoids have potent immunosuppressive effects, their application in ALI is currently being tested in clinical trials. However, the benefits of this type of regimen remain unclear. Here we identify a mechanism of glucocorticoid action that challenges the long-standing dogma of cytokine repression by the glucocorticoid receptor. Contrarily, synergistic gene induction of sphingosine kinase 1 (SphK1) by glucocorticoids and pro-inflammatory stimuli via the glucocorticoid receptor in macrophages increases circulating sphingosine 1-phosphate levels, which proves essential for the inhibition of inflammation. Chemical or genetic inhibition of SphK1 abrogates the therapeutic effects of glucocorticoids. Inflammatory p38 MAPK- and mitogen- and stress-activated protein kinase 1 (MSK1)-dependent pathways cooperate with glucocorticoids to upregulate SphK1 expression. Our findings support a critical role for SphK1 induction in the suppression of lung inflammation by glucocorticoids, and therefore provide rationales for effective anti-inflammatory therapies.

Published

2015