Your search keyword '"Schnautz, Benjamin"' showing total 9 results

1. Pinewood VOC emissions protect from oxazolone-induced inflammation and dysbiosis in a mouse model of atopic dermatitis

Author

Schneider, Evelyn, Amar, Yacine, Butter, Katja, Steiger, Katja, Musiol, Stephanie, Garcia-Käufer, Manuel, Hölge, Inga Marie, Schnautz, Benjamin, Gschwendtner, Silvia, Ghirardo, Andrea, Gminski, Richard, Eberlein, Bernadette, Esser von Bieren, Julia, Biedermann, Tilo, Haak, Stefan, Ohlmeyer, Martin, Schmidt-Weber, Carsten B., Eyerich, Stefanie, and Alessandrini, Francesca

Published

2024

2. Ex Vivo Immunomodulatory Effects of Lactobacillus-, Lacticaseibacillus-, and Bifidobacterium-Containing Synbiotics on Human Peripheral Blood Mononuclear Cells and Monocyte-Derived Dendritic Cells in the Context of Grass Pollen Allergy

Author

Heldner, Alexander, Heath, Matthew D., Schnautz, Benjamin, Kotz, Sebastian, Chaker, Adam, Kramer, Matthias F., Jakwerth, Constanze A., Zissler, Ulrich M., Schmidt-Weber, Carsten B., and Blank, Simon

Published

2023

3. The impact of high‐salt diet on asthma in humans and mice: Effect on specific T‐cell signatures and microbiome.

Author

Musiol, Stephanie, Harris, Carla P., Gschwendtner, Silvia, Burrell, Amy, Amar, Yacine, Schnautz, Benjamin, Renisch, Dennis, Braun, Sonja C., Haak, Stefan, Schloter, Michael, Schmidt‐Weber, Carsten B., Zielinski, Christina E., and Alessandrini, Francesca

Subjects

HIGH-salt diet, SHORT-chain fatty acids, ASTHMA, DIETARY patterns, T cells, ATOPY

Abstract

Background: The rise in asthma has been linked to different environmental and lifestyle factors including dietary habits. Whether dietary salt contributes to asthma incidence, remains controversial. We aimed to investigate the impact of higher salt intake on asthma incidence in humans and to evaluate underlying mechanisms using mouse models. Methods: Epidemiological research was conducted using the UK Biobank Resource. Data were obtained from 42,976 participants with a history of allergies. 24‐h sodium excretion was estimated from spot urine, and its association with asthma incidence was assessed by Cox regression, adjusting for relevant covariates. For mechanistic studies, a mouse model of mite‐induced allergic airway inflammation (AAI) fed with high‐salt diet (HSD) or normal‐salt chow was used to characterize disease development. The microbiome of lung and feces (as proxy for gut) was analyzed via 16S rRNA gene based metabarcoding approach. Results: In humans, urinary sodium excretion was directly associated with asthma incidence among females but not among males. HSD‐fed female mice displayed an aggravated AAI characterized by increased levels of total IgE, a TH2‐TH17‐biased inflammatory cell infiltration accompanied by upregulation of osmosensitive stress genes. HSD induced distinct changes in serum short chain fatty acids and in both gut and lung microbiome, with a lower Bacteroidetes to Firmicutes ratio and decreased Lactobacillus relative abundance in the gut, and enriched members of Gammaproteobacteria in the lung. Conclusions: High dietary salt consumption correlates with asthma incidence in female adults with a history of allergies. Female mice revealed HSD‐induced T‐cell lung profiles accompanied by alterations of gut and lung microbiome. [ABSTRACT FROM AUTHOR]

Published

2024

4. Activation of the aryl hydrocarbon receptor improves allergen-specific immunotherapy of murine allergic airway inflammation: a novel adjuvant option?

Author

Heine, Sonja, Alessandrini, Francesca, Grosch, Johannes, Graß, Carina, Heldner, Alexander, Schnautz, Benjamin, Grosch, Johanna, Buters, Jeroen, Slusarenko, Benjamin O., Krappmann, Daniel, Fallarino, Francesca, Ohnmacht, Caspar, Schmidt-Weber, Carsten B., and Blank, Simon

Subjects

ARYL hydrocarbon receptors, TRANSCRIPTION factors, TREATMENT effectiveness, IMMUNOTHERAPY, TH2 cells

Abstract

Background: Allergen-specific immunotherapy (AIT) is able to restore immune tolerance to allergens in allergic patients. However, some patients do not or only poorly respond to current treatment protocols. Therefore, there is a need for deeper mechanistic insights and further improvement of treatment strategies. The relevance of the aryl hydrocarbon receptor (AhR), a ligand-dependent transcription factor, has been investigated in several inflammatory diseases, including allergic asthma. However, its potential role in AIT still needs to be addressed. Methods: Amurinemodel of AIT in ovalbumin-induced allergic airway inflammation was performed in AhR-deficient (AhR-/-) and wild-type mice. Furthermore, AIT was combined with the application of the high-affinity AhR agonist 10-chloro-7Hbenzimidazo[2,1-a]benzo[de]iso-quinolin-7-one (10-Cl-BBQ) as an adjuvant to investigate the effects of AhR activation on therapeutic outcome. Results: Although AhR-/- mice suffer stronger allergic responses than wild-type mice, experimental AIT is comparably effective in both. Nevertheless, combining AIT with the administration of 10-Cl-BBQ improved therapeutic effects by an AhRdependent mechanism, resulting in decreased cell counts in the bronchoalveolar fluid, decreased pulmonary Th2 and Th17 cell levels, and lower sIgE levels. Conclusion: This study demonstrates that the success of AIT is not dependent on the AhR. However, targeting the AhR during AIT can help to dampen inflammation and improve tolerogenic vaccination. Therefore, AhR ligands might represent promising candidates as immunomodulators to enhance the efficacy of AIT. [ABSTRACT FROM AUTHOR]

Published

2024

5. The aryl hydrocarbon receptor regulates lipid mediator production in alveolar macrophages.

Author

Maier, Ann-Marie, Huth, Karsten, Alessandrini, Francesca, Henkel, Fiona, Schnautz, Benjamin, Arifovic, Anela, Riols, Fabien, Haid, Mark, Koegler, Anja, Sameith, Katrin, Schmidt-Weber, Carsten B., Esser-von-Bieren, Julia, and Ohnmacht, Caspar

Subjects

ARYL hydrocarbon receptors, ALVEOLAR macrophages, LIQUID chromatography-mass spectrometry, LIPOXINS, OXYGENASES, HOUSE dust mites, EPITHELIAL cells

Abstract

Allergic inflammation of the airways such as allergic asthma is a major health problem with growing incidence world-wide. One cardinal feature in severe type 2-dominated airway inflammation is the release of lipid mediators of the eicosanoid family that can either promote or dampen allergic inflammation. Macrophages are key producers of prostaglandins and leukotrienes which play diverse roles in allergic airway inflammation and thus require tight control. Using RNA- and ATAC-sequencing, liquid chromatography coupled to mass spectrometry (LC-MS/MS), enzyme immunoassays (EIA), gene expression analysis and in vivo models, we show that the aryl hydrocarbon receptor (AhR) contributes to this control via transcriptional regulation of lipid mediator synthesis enzymes in bone marrow-derived as well as in primary alveolar macrophages. In the absence or inhibition of AhR activity, multiple genes of both the prostaglandin and the leukotriene pathway were downregulated, resulting in lower synthesis of prostanoids, such as prostaglandin E2 (PGE2), and cysteinyl leukotrienes, e.g., Leukotriene C4 (LTC4). These AhR-dependent genes include PTGS1 encoding for the enzyme cyclooxygenase 1 (COX1) and ALOX5 encoding for the arachidonate 5-lipoxygenase (5-LO) both of which major upstream regulators of the prostanoid and leukotriene pathway, respectively. This regulation is independent of the activation stimulus and partially also detectable in unstimulated macrophages suggesting an important role of basal AhR activity for eicosanoid production in steady state macrophages. Lastly, we demonstrate that AhR deficiency in hematopoietic but not epithelial cells aggravates house dust mite induced allergic airway inflammation. These results suggest an essential role for AhR-dependent eicosanoid regulation in macrophages during homeostasis and inflammation. [ABSTRACT FROM AUTHOR]

Published

2023

6. Dietary digestible carbohydrates are associated with higher prevalence of asthma in humans and with aggravated lung allergic inflammation in mice.

Author

Musiol, Stephanie, Harris, Carla P., Karlina, Ruth, Gostner, Johanna M., Rathkolb, Birgit, Schnautz, Benjamin, Schneider, Evelyn, Mair, Lisa, Vergara, Ernesto Elorduy, Flexeder, Claudia, Koletzko, Sibylle, Bauer, Carl‐Peter, Schikowski, Tamara, Berdel, Dietrich, von Berg, Andrea, Herberth, Gunda, Rozman, Jan, Hrabe de Angelis, Martin, Standl, Marie, and Schmidt‐Weber, Carsten B.

Subjects

DIETARY carbohydrates, PNEUMONIA, DIETARY sucrose, WHEEZE, ASTHMA, DIETARY fats, ALLERGIC conjunctivitis

Abstract

Background: Dietary carbohydrates and fats are intrinsically correlated within the habitual diet. We aimed to disentangle the associations of starch and sucrose from those of fat, in relation to allergic sensitization, asthma and rhinoconjuctivitis prevalence in humans, and to investigate underlying mechanisms using murine models. Methods: Epidemiological data from participants of two German birth cohorts (age 15) were used in logistic regression analyses testing cross‐sectional associations of starch and sucrose (and their main dietary sources) with aeroallergen sensitization, asthma and rhinoconjunctivitis, adjusting for correlated fats (saturated, monounsaturated, omega‐6 and omega‐3 polyunsaturated) and other covariates. For mechanistic insights, murine models of aeroallergen‐induced allergic airway inflammation (AAI) fed with a low‐fat‐high‐sucrose or ‐high‐starch versus a high‐fat diet were used to characterize and quantify disease development. Metabolic and physiologic parameters were used to track outcomes of dietary interventions and cellular and molecular responses to monitor the development of AAI. Oxidative stress biomarkers were measured in murine sera or lung homogenates. Results: We demonstrate a direct association of dietary sucrose with asthma prevalence in males, while starch was associated with higher asthma prevalence in females. In mice, high‐carbohydrate feeding, despite scant metabolic effects, aggravated AAI compared to high‐fat in both sexes, as displayed by humoral response, mucus hypersecretion, lung inflammatory cell infiltration and TH2‐TH17 profiles. Compared to high‐fat, high‐carbohydrate intake was associated with increased pulmonary oxidative stress, signals of metabolic switch to glycolysis and decreased systemic anti‐oxidative capacity. Conclusion: High consumption of digestible carbohydrates is associated with an increased prevalence of asthma in humans and aggravated lung allergic inflammation in mice, involving oxidative stress‐related mechanisms. [ABSTRACT FROM AUTHOR]

Published

2023

7. Immunological effects of adjuvanted low‐dose allergoid allergen‐specific immunotherapy in experimental murine house dust mite allergy.

Author

Heldner, Alexander, Alessandrini, Francesca, Russkamp, Dennis, Heine, Sonja, Schnautz, Benjamin, Chaker, Adam, Mwange, Juliet, Carreno Velazquez, Thalia L., Heath, Matthew D., Skinner, Murray A., Kramer, Matthias F., Zissler, Ulrich M., Schmidt‐Weber, Carsten B., and Blank, Simon

Subjects

HOUSE dust mites, ALLERGENIC extracts, ALLERGIES, THERAPEUTICS, IMMUNOTHERAPY

Abstract

Background: Native allergen extracts or chemically modified allergoids are routinely used to induce allergen tolerance in allergen‐specific immunotherapy (AIT), although mechanistic side‐by‐side studies are rare. It is paramount to balance optimal dose and allergenicity to achieve efficacy warranting safety. AIT safety and efficacy could be addressed by allergen dose reduction and/or use of allergoids and immunostimulatory adjuvants, respectively. In this study, immunological effects of experimental house dust mite (HDM) AIT were investigated applying high‐dose HDM extract and low‐dose HDM allergoids with and without the adjuvants microcrystalline tyrosine (MCT) and monophosphoryl lipid A (MPL) in a murine model of HDM allergy. Methods: Cellular, humoral, and clinical effects of the different AIT strategies were assessed applying a new experimental AIT model of murine allergic asthma based on physiological, adjuvant‐free intranasal sensitization followed by subcutaneous AIT. Results: While low‐dose allergoid and high‐dose extract AIT demonstrated comparable potency to suppress allergic airway inflammation and Th2‐type cytokine secretion of lung‐resident lymphocytes and draining lymph node cells, low‐dose allergoid AIT was less effective in inducing a potentially protective IgG1 response. Combining low‐dose allergoid AIT with MCT or MCT and dose‐adjusted MPL promoted Th1‐inducing mechanisms and robust B‐cell activation counterbalancing the allergic Th2 immune response. Conclusion: Low allergen doses induce cellular and humoral mechanisms counteracting Th2‐driven inflammation by using allergoids and dose‐adjusted adjuvants. In light of safety and efficacy improvement, future therapeutic approaches may use low‐dose allergoid strategies to drive cellular tolerance and adjuvants to modulate humoral responses. [ABSTRACT FROM AUTHOR]

Published

2022

8. TGF-β1 Drives Inflammatory Th Cell But Not Treg Cell Compartment Upon Allergen Exposure.

Author

Musiol, Stephanie, Alessandrini, Francesca, Jakwerth, Constanze A., Chaker, Adam M., Schneider, Evelyn, Guerth, Ferdinand, Schnautz, Benjamin, Grosch, Johanna, Ghiordanescu, Ileana, Ullmann, Julia T., Kau, Josephine, Plaschke, Mirjam, Haak, Stefan, Buch, Thorsten, Schmidt-Weber, Carsten B., and Zissler, Ulrich M.

Subjects

REGULATORY T cells, T helper cells, T cells, ALLERGENS, TH2 cells

Abstract

TGF-β1 is known to have a pro-inflammatory impact by inducing Th9 and Th17 cells, while it also induces anti-inflammatory Treg cells (Tregs). In the context of allergic airway inflammation (AAI) its dual role can be of critical importance in influencing the outcome of the disease. Here we demonstrate that TGF-β is a major player in AAI by driving effector T cells, while Tregs differentiate independently. Induction of experimental AAI and airway hyperreactivity in a mouse model with inducible genetic ablation of the gene encoding for TGFβ-receptor 2 (Tgfbr2) on CD4+T cells significantly reduced the disease phenotype. Further, it blocked the induction of pro-inflammatory T cell frequencies (Th2, Th9, Th17), but increased Treg cells. To translate these findings into a human clinically relevant context, Th2, Th9 and Treg cells were quantified both locally in induced sputum and systemically in blood of allergic rhinitis and asthma patients with or without allergen-specific immunotherapy (AIT). Natural allergen exposure induced local and systemic Th2, Th9, and reduced Tregs cells, while therapeutic allergen exposure by AIT suppressed Th2 and Th9 cell frequencies along with TGF-β and IL-9 secretion. Altogether, these findings support that neutralization of TGF-β represents a viable therapeutic option in allergy and asthma, not posing the risk of immune dysregulation by impacting Tregs cells. [ABSTRACT FROM AUTHOR]

Published

2022

9. Corrigendum: The aryl hydrocarbon receptor regulates lipid mediator production in alveolar macrophages.

Author

Maier AM, Huth K, Alessandrini F, Henkel F, Schnautz B, Arifovic A, Riols F, Haid M, Koegler A, Sameith K, Schmidt-Weber CB, Esser-von-Bieren J, and Ohnmacht C

Abstract

[This corrects the article DOI: 10.3389/fimmu.2023.1157373.]., (Copyright © 2023 Maier, Huth, Alessandrini, Henkel, Schnautz, Arifovic, Riols, Haid, Koegler, Sameith, Schmidt-Weber, Esser-von-Bieren and Ohnmacht.)

Published

2023