Your search keyword '"Gutermuth, Jan"' showing total 160 results

151. Analyse der IgE mediierten Autoreaktivität bei atopischen Erkrankungen bei Kindern und Erwachsenen

Author

Seher, Tanja, Schmidt-Weber, Carsten (Prof. Dr.), Groß, Olaf (Priv.-Doz. Dr.), and Gutermuth, Jan (Prof. Dr.)

Subjects

Medizin und Gesundheit, autoreaktives IgE, Asthma, atopisches Ekzem, Alelrgie, Autoimmunität, autoreactive IgE, asthma, atopic eczema, allergy, autoimmunity, ddc:610

Abstract

Background: Atopic diseases are IgE-mediated and bear an immunologic reaction towards usually innocuous environmental factors to what healthy subjects are tolerant. Atopic diseases can manifest and pass into chronic forms particularly atopic eczema and allergic asthma. The cause of the manifestation is rather ambiguous; furthermore it is unclear why atopy manifests in some individuals but not others, although the exposure to environmental allergens is similar. One hypothesis is the occurrence of autoreactive IgE that targets primarily tissues and cells of allergic inflammation. Due to tissue damage intracellular proteins are released and recognized by autoreactive IgE antibodies. However, if auto-IgE is cross-reactive to human self-proteins or whether it is produced by neo-synthesis subsequently to autosensitization is not clear so far. Methods: We established a high-throughput immunoassay in 384-well format to screen auto-IgE in serum. As target protein we used whole cell protein of keratinocytes, bronchial epithelial cells. We investigated adult atopic patients with different skin diseases as atopic eczema or asthma to figure out whether those patients have higher quantity of auto-IgE in serum. A small group of patients with heterogenous age having atopic eczema was analyzed initially, before we investigated children at the age of ten out from the GINI/LISA birth cohorts to reveal whether auto-IgE is generated physiologically and if auto-IgE is associated with atopic diseases in infancy. Results: We observed two different properties of auto-IgE in two periods of life. During childhood auto-IgE was generated physiologically and there is evidence that auto-IgE is a natural occurring antibody. No association of clinical manifestation of atopy and auto-IgE in children could be assessed. Furthermore, sensitization enhanced the quantity of auto-IgE reactivity and there is evidence that the occurrence of auto-IgE is protective towards eczema. In contrast, adults having atopic eczema showed more frequent and higher auto-IgE reactivity. In asthmatic patients auto-IgE reactivity was significantly associated with the control status of the disease. The less asthma was controlled the higher the auto-IgE reactivity. Healthy adult subjects do not show auto-IgE reactivity. Conclusion: The study indicates dissimilarities of autoreactive IgE between childhood and adulthood. Whereas auto-IgE seems to represent a natural response that is not necessarily associated with pathology in childhood, the occurrence of auto-IgE is disease associated in adults and one can assume a pathomechanistic effect in adult atopic patients. Based on these new aspects of auto-IgE the present study represents fairly new aspects on autoallergy. One can assume a pathomechanistic effect in adult atopic patients. Hintergrund: Atopische Erkrankungen sind IgE-mediiert und durch eine überschießende immunologische Reaktion gegen harmlose Umweltfaktoren charakterisiert. Die Ursache der Chronifizierung atopischer Erkrankungen, wie sie häufiger beim atopischen Ekzem und beim allergischen Asthma auftritt ist unbekannt. Ebenfalls unbekannt ist, warum die Erkrankung bei einigen Patienten chronifiziert und bei anderen nicht. Eine Hypothese ist das Auftreten autoreaktiver IgE-Antikörper. Bereits zu Beginn der allergischen Inflammation kommt es zum Barrierebruch und zur Gewebsschädigung wodurch zelluläre Proteine freigesetzt werden, die dem auto-IgE Antikörper als Targetproteine dienen. Bisher ist unklar, ob autoreaktive IgE-Antikörper einen pathomechanistischen Einfluss auf die Aggravation und Chronifizierung atopischer Erkrankungen haben oder ob es sich um ein Epiphänomen handelt. Methode: Für den Nachweis autoreaktiver IgE Antikörper haben wir einen Immunoassay im 384-well Format etabliert. Für diesen nutzten wir Gesamtzellprotein von Keratinozyten (HaCaT-Zelllinie) und von primären Bronchialzellen als Targetprotein. Wir untersuchten Patienten mit unterschiedlichen Hauterkrankungen (z.B. atopisches Ekzem), sowie adulte Asthmatiker und Kinder im Alter von 10 Jahren aus den GINI und LISA Geburtskohorten. Ergebnisse: Autoreaktives IgE zeigt unterschiedliche Charaktere im Kind und beim Erwachsenen. Im Kind ist das Vorkommen von auto-IgE physiologisch und nicht mit atopischen Erkrankungen assoziiert. Im Adulten hingegen ist auto-IgE positiv mit dem atopischen Ekzem und Asthma assoziiert. Des Weiteren lässt sich sagen, je schlechter das Asthma kontrolliert ist, desto höher ist die auto-IgE Reaktivität. In gesunden Erwachsenen liegt in dieser Studie kein physiologisches auto-IgE vor. Schlussfolgerung: Die Studie zeigt erstmals die Divergenz des auto-IgE bei Erwachsenen und Kindern. Das physiologische Vorliegen von auto-IgE im Kindesalter deutet auf einen natürlichen Autoantikörper hin, indessen im Erwachsenenalter das Vorkommen mit atopischen Erkrankungen assoziiert ist, was möglicherweise auf einen pathomechanistischen Effekt hindeutet.

Published

2016

152. Analysis of the sensitizing properties of ragweed pollen components and the influence of environmental factors in a murine in vivo model

Author

Kamml, Maria, Gutermuth, Jan (Prof. Dr.), and Durner, Jörg (Prof. Dr.)

Subjects

Medizin und Gesundheit, otorhinolaryngologic diseases, ddc:610, Ambrosia artemisiifolia, Traubenkraut, Pollen, Allergie, Sensibilisierung, Adjuvans, Adenosin, Ragweed, Ambrosia artemisiifolia, pollen, allergy, sensitization, adjuvant, adenosine

Abstract

Ragweed is an environmentally relevant neo-allergen in Europe. Using a murine sensitization model, the allergenic potential of ragweed pollen grown under elevated ozone levels was analyzed. Furthermore, in a physiological sensitization model via the nasal mucosa the sensitizing properties of total ragweed pollen extract, its protein-free fraction, and of the major allergen Amb a 1 were evaluated. Moreover, adenosine, a low-molecular weight substance contained in high amounts in the protein-fee fraction of ragweed pollen extract, was investigated for its role in sensitization. Ambrosia ist ein umweltrelevantes Allergen in Europa. Mittels eines murinen Sensibilisierungsmodells wurde das allergene Potential von Ambrosiapollen, die unter erhöhten Ozonbedingungen gewachsen sind, analysiert. In einem physiologischen Sensibilisierungsmodell über die Nasenschleimhaut wurden die sensibilisierenden Eigenschaften des Gesamtambrosiapollen-Extraktes, dessen proteinfreier Fraktion und des Hauptallergens Amb a 1 bewertet. Außerdem wurde die Rolle von Adenosin, das in hohen Mengen im Ambrosiapollen-Extrakt enthalten ist, in der Sensibilisierung untersucht.

Published

2015

153. Navigating the evolving landscape of atopic dermatitis: Challenges and future opportunities: The 4th Davos declaration.

Author

Traidl-Hoffmann C, Afghani J, Akdis CA, Akdis M, Aydin H, Bärenfaller K, Behrendt H, Bieber T, Bigliardi P, Bigliardi-Qi M, Bonefeld CM, Bösch S, Brüggen MC, Diemert S, Duchna HW, Fähndrich M, Fehr D, Fellmann M, Frei R, Garvey LH, Gharbo R, Gökkaya M, Grando K, Guillet C, Guler E, Gutermuth J, Herrmann N, Hijnen DJ, Hülpüsch C, Irvine AD, Jensen-Jarolim E, Kong HH, Koren H, Lang CCV, Lauener R, Maintz L, Mantel PY, Maverakis E, Möhrenschlager M, Müller S, Nadeau K, Neumann AU, O'Mahony L, Rabenja FR, Renz H, Rhyner C, Rietschel E, Ring J, Roduit C, Sasaki M, Schenk M, Schröder J, Simon D, Simon HU, Sokolowska M, Ständer S, Steinhoff M, Piccirillo DS, Taïeb A, Takaoka R, Tapparo M, Teixeira H, Thyssen JP, Traidl S, Uhlmann M, van de Veen W, van Hage M, Virchow C, Wollenberg A, Yasutaka M, Zink A, and Schmid-Grendelmeier P

Subjects

Humans, Disease Management, Dermatitis, Atopic therapy

Abstract

The 4th Davos Declaration was developed during the Global Allergy Forum in Davos which aimed to elevate the care of patients with atopic dermatitis (AD) by uniting experts and stakeholders. The forum addressed the high prevalence of AD, with a strategic focus on advancing research, treatment, and management to meet the evolving challenges in the field. This multidisciplinary forum brought together top leaders from research, clinical practice, policy, and patient advocacy to discuss the critical aspects of AD, including neuroimmunology, environmental factors, comorbidities, and breakthroughs in prevention, diagnosis, and treatment. The discussions were geared towards fostering a collaborative approach to integrate these advancements into practical, patient-centric care. The forum underlined the mounting burden of AD, attributing it to significant environmental and lifestyle changes. It acknowledged the progress in understanding AD and in developing targeted therapies but recognized a gap in translating these innovations into clinical practice. Emphasis was placed on the need for enhanced awareness, education, and stakeholder engagement to address this gap effectively and to consider environmental and lifestyle factors in a comprehensive disease management strategy. The 4th Davos Declaration marks a significant milestone in the journey to improve care for people with AD. By promoting a holistic approach that combines research, education, and clinical application, the Forum sets a roadmap for stakeholders to collaborate to improve patient outcomes in AD, reflecting a commitment to adapt and respond to the dynamic challenges of AD in a changing world., (© 2024 The Author(s). Allergy published by European Academy of Allergy and Clinical Immunology and John Wiley & Sons Ltd.)

Published

2024

154. Improvement in Early Scar Maturation by Nanofat Infiltration: Histological and Spectrophotometric Preliminary Results From a Split Scar-Controlled, Randomized, Double-Blinded Clinical Trial.

Author

Ramaut L, Moonen L, Geeroms M, Leemans G, Peters E, Forsyth R, Gutermuth J, and Hamdi M

Abstract

Background: The regenerative properties of stromal vascular fraction (SVF) in wound healing and scar formation are a subject of increasing clinical interest., Objectives: Although preclinical studies have confirmed the angiogenetic, proliferative, and antifibrotic properties of SVF, there is limited clinical evidence from randomized controlled clinical trials., Methods: Twelve patients who underwent abdominoplasty were included in this clinical study. Nanofat was mechanically obtained intraoperatively and infiltrated intradermally in the sutured surgical wound, randomly assigned to either the left or the right side. The abdominal scar was evaluated with the Patient and Observer Scar Assessment Scale, whereas erythema and pigmentation were measured with a reflectance spectrophotometry device (Mexameter, Courage + Khazaka electronic GmbH, Köln,Germany). Histological analysis and electron scan microscopy of tissue biopsies were performed at 8 months., Results: The treated side of the scar showed significantly less erythema at 3- and 6-month follow-ups, but this difference reduced after 12 months. Patients reported better scar scores at the 6-month follow-up with a significantly better color at the treated side. Observers reported better overall scar scores at the treated side at 3-, 6-, and 12-month follow-ups, with better vascularization, pigmentation, and thickness. There was no statistically significant difference in terms of histological analysis between the 2 groups. There was no difference in the occurrence of adverse events between both sides., Conclusions: Infiltration of nanofat exhibited promising results in surgical scar maturation characterized by less erythema and better texture. More clinical trials with a larger sample size are warranted to better elucidate the possible benefits of SVF on surgical scar formation., (© The Author(s) 2024. Published by Oxford University Press on behalf of The Aesthetic Society.)

Published

2024

155. Value-Based Healthcare: A Primer for the Dermatologist.

Author

Balak DMW, Deprez E, Hilhorst NT, Hoorens I, Gutermuth J, Bos WJW, and Lambert J

Abstract

Background: Value-based healthcare (VBHC) is an increasingly employed strategy to transform healthcare organizations into economically sustainable systems that deliver high-value care. In dermatology, the need for VBHC is evident as chronic skin diseases require long-term, often expensive treatments. This narrative review aims to introduce dermatologists to the principles and implementation of VBHC., Summary: VBHC emphasizes maximizing outcomes that are directly relevant to patients. Key components of VBHC include a systematic assessment of standardized patient-relevant outcomes by using core outcome sets and measurement of healthcare cost for the individual patient. Systematic reporting and comparing of risk-adjusted outcomes across the full cycle of care for a specific condition provide benchmarked feedback and actionable insights to promote high-value care and reduce low-value care. VBHC aims to organize care around the patient in condition-specific and team-based integrated practice units with multidisciplinary collaboration, utilize information technology platforms to enable digital data monitoring, reduce cost, and eventually reform payment systems to support bundled payments for the overall care cycle. VBHC implementation in practice necessitates the establishment of a systematic framework for outcome-based quality improvement, the incorporation of value and outcomes in shared decision-making practices, and the cultivation of a value-centric culture among healthcare professionals through continuous training., Key Messages: Dermatologists can benefit from implementing VBHC principles in their practice. An essential step toward value-driven dermatological care is to start measuring outcomes relevant for patients for each patient, which is lacking partly due to the absence of core outcome sets developed for clinical practice. By reducing low-value care and emphasizing optimal patient-centered outcomes, VBHC has the potential to improve the quality of care and ensure cost containment. Efforts are needed to enhance the development and uptake of VBHC in dermatological clinical practice to realize these benefits., (© 2024 The Author(s). Published by S. Karger AG, Basel.)

Published

2024

156. A red, bumpy back in a neonate.

Author

Hillary T, Huysentruyt K, De Coninck A, Gutermuth J, De Raeve L, and Cools F

Published

2016

157. Rote Beulen am Rücken eines Neugeborenen.

Author

Hillary T, Huysentruyt K, De Coninck A, Gutermuth J, De Raeve L, and Cools F

Published

2016

158. [Intracutaneous nodules in a three-year-old girl. Leukemia cutis].

Author

Onken AT, Westphal S, Schnopp C, Ring J, Ollert M, Gutermuth J, and Andres C

Subjects

Child, Preschool, Diagnosis, Differential, Female, Humans, Leukemia, Myeloid, Acute pathology, Skin Neoplasms pathology

Published

2012

159. Self-peptides prolong survival in murine autoimmunity via reduced IL-2/IL-7-mediated STAT5 signaling, CD8 coreceptor, and V alpha 2 down-regulation.

Author

Gutermuth J, Nograles KE, Miyagawa F, Nelson E, Cho YH, and Katz SI

Subjects

Animals, Autoimmune Diseases immunology, Autoimmune Diseases mortality, CD8 Antigens metabolism, Chickens, Clonal Anergy genetics, Clonal Anergy immunology, Down-Regulation genetics, Immune Tolerance genetics, Interleukin-2 physiology, Interleukin-7 physiology, Mice, Mice, Inbred C57BL, Mice, Knockout, Mice, Transgenic, Ovalbumin administration & dosage, Ovalbumin genetics, Ovalbumin immunology, Peptide Fragments administration & dosage, Peptide Fragments genetics, Peptide Fragments immunology, Receptors, Antigen, T-Cell metabolism, Receptors, Antigen, T-Cell, alpha-beta biosynthesis, STAT5 Transcription Factor metabolism, STAT5 Transcription Factor physiology, Signal Transduction genetics, Solubility, Survival Analysis, Autoimmune Diseases therapy, Down-Regulation immunology, Interleukin-2 antagonists & inhibitors, Interleukin-7 antagonists & inhibitors, Ovalbumin physiology, Peptide Fragments physiology, Receptors, Antigen, T-Cell antagonists & inhibitors, Receptors, Antigen, T-Cell, alpha-beta antagonists & inhibitors, STAT5 Transcription Factor antagonists & inhibitors, Signal Transduction immunology

Abstract

Although the pathogenic role of B cells and CD4 T cells has been studied extensively, less is known about the role of CD8 T cells in autoimmunity and self-tolerance. To evaluate the role of CD8 T cells in autoimmunity and its modulation using self-peptides, we used mice expressing soluble OVA (sOVA) under control of the keratin-14 promoter. Spontaneous autoimmunity occurred when sOVA mice were crossed with OT-I mice, whose CD8 T cells carry a Valpha2/Vbeta5-transgenic TCR with specificity for the OVA(257-264) peptide. Eighty-three percent of OVA/OT-I mice died during the first 2 wk of life due to multiple organ inflammation. In contrast, preventive or therapeutic OVA(257-264) peptide injections induced a dose-dependent increase in survival. Healthy survivors exhibited reductions in peripheral CD8 T cells, CD8 coreceptor, and Valpha2 expression. Furthermore, CD8 T cells from healthy mice were anergic and could not be activated by exogenous IL-2. A block in IL-2/IL-7 signaling via the STAT5 pathway provided the basis for low surface expression of the CD8 coreceptor and failure of IL-2 to break CD8 T cell anergy. Thus, the soluble TCR ligand triggered multiple tolerance mechanisms in these sOVA/OT-I mice, making this treatment approach a potential paradigm for modulating human autoimmune diseases.

Published

2009

160. The Bcl10-Malt1 complex segregates Fc epsilon RI-mediated nuclear factor kappa B activation and cytokine production from mast cell degranulation.

Author

Klemm S, Gutermuth J, Hültner L, Sparwasser T, Behrendt H, Peschel C, Mak TW, Jakob T, and Ruland J

Subjects

Adaptor Proteins, Signal Transducing deficiency, Adaptor Proteins, Signal Transducing genetics, Animals, B-Cell CLL-Lymphoma 10 Protein, Caspases, Cells, Cultured, Immunoglobulin E physiology, Lipid Metabolism genetics, Lipid Metabolism immunology, Lymphoma, B-Cell, Marginal Zone genetics, Mast Cells metabolism, Mice, Mice, Inbred C57BL, Mice, Knockout, Mucosa-Associated Lymphoid Tissue Lymphoma Translocation 1 Protein, Multiprotein Complexes deficiency, Multiprotein Complexes genetics, Neoplasm Proteins deficiency, Neoplasm Proteins genetics, Adaptor Proteins, Signal Transducing physiology, Cell Degranulation immunology, Cytokines biosynthesis, Mast Cells immunology, Multiprotein Complexes physiology, NF-kappa B metabolism, Neoplasm Proteins physiology, Receptors, IgE physiology

Abstract

Mast cells are pivotal effector cells in IgE-mediated allergic inflammatory diseases. Central for mast cell activation are signals from the IgE receptor FcepsilonRI, which induce cell degranulation with the release of preformed mediators and de novo synthesis of proinflammatory leukotrienes and cytokines. How these individual mast cell responses are differentially controlled is still unresolved. We identify B cell lymphoma 10 (Bcl10) and mucosa-associated lymphoid tissue 1 (Malt1) as novel key regulators of mast cell signaling. Mice deficient for either protein display severely impaired IgE-dependent late phase anaphylactic reactions. Mast cells from these animals neither activate nuclear factor kappaB (NF-kappaB) nor produce tumor necrosis factor alpha or interleukin 6 upon FcepsilonRI ligation even though proximal signaling, degranulation, and leukotriene secretion are normal. Thus, Bcl10 and Malt1 are essential positive mediators of FcepsilonRI-dependent mast cell activation that selectively uncouple NF-kappaB-induced proinflammatory cytokine production from degranulation and leukotriene synthesis.

Published

2006