Your search keyword '"Kunz, Stefanie"' showing total 7 results

1. Contact allergens induce CD8+ T cell-derived interleukin 10 that appears dispensable for regulation of contact hypersensitivity.

Author

Dolch, Anja, Kunz, Stefanie, Dorn, Britta, Roers, Axel, Martin, Stefan F., and Jakob, Thilo

Subjects

*CONTACT dermatitis, *ALLERGENS, *CD8 antigen, *INTERLEUKIN-10, *IMMUNOREGULATION, *PREVENTION

Abstract

Interleukin 10 ( IL-10) has been implied in the regulation of allergic contact dermatitis. Using transcriptional reporter mice we analyzed cellular sources of IL-10 during contact hypersensitivity ( CHS) and identified IL-10 expressing CD8+ T cells in the skin that are antigen-specific, display PD-1, an effector memory phenotype, and IL-10 expression comparable to that of CD4+ T cells. However, in mice with a selective IL-10 deficiency in CD8+ T cells CHS responses were comparable to that of controls, even in the absence of CD4+ cells, suggesting that CD8+ T cell-derived IL-10 does not contribute significantly to the resolution of CHS responses. [ABSTRACT FROM AUTHOR]

Published

2017

2. Interleukin (IL)-19, IL-20 and IL-24 are produced by and act on keratinocytes and are distinct from classical ILs.

Author

Kunz, Stefanie, Wolk, Kerstin, Witte, Ellen, Witte, Katrin, Doecke, Wolf-Dietrich, Volk, Hans-Dieter, Sterry, Wolfram, Asadullah, Khusru, and Sabat, Robert

Subjects

*INTERLEUKINS, *GENE expression, *KERATINOCYTES, *INFLAMMATORY mediators, *LYMPH nodes, *DENDRITIC cells, *TISSUES

Abstract

Due to their structural similarity, interleukin (IL)-19, IL-20, IL-22, IL-24 and IL-26 were combined with IL-10 in the so-called IL-10 family. To expand the knowledge on IL-19, IL-20 and IL-24, we systematically and quantitatively analysed the expression of these mediators and their receptor chains in vitro and in vivo under various conditions and in comparison with other IL-10 family members. In vitro, IL-19, IL-20 and IL-24 were produced not only by activated immune cells, particularly monocytes, but also to a similar extent by keratinocytes. IL-1 β increased the expression of these mediators 1000-fold (IL-19) and 10-fold (IL-20 and IL-24) in keratinocytes. In vivo, these cytokines were expressed preferentially in inflamed tissues. The absence of either R1 chain for the two types of receptor complexes for these cytokines (IL-20R1/IL-20R2 and IL-22R1/IL-20R2) on immune cells implies that they cannot act on these cells. In fact, IL-19, IL-20 and IL-24 did not induce activation of signal transducer and activator of transcription (STAT) molecules in immune cells. Instead, several tissues, particularly the skin, tissues from the reproductive and respiratory systems, and various glands appeared to be the main targets of these mediators. Keratinocytes expressed both receptor complexes; however, the expression of IL-22R1 was 10 times higher than that of IL-20R1. Interferon- γ further increased the expression of IL-22R1 and decreased that of IL-20R1, suggesting that under T1 cytokine conditions these mediators primarily affect keratinocytes via the IL-22R1/IL-20R2 complex. In summary, these data support the notion that IL-19, IL-20 and IL-24 are distinct from classical ILs and constitute a separate subfamily of mediators within the IL-10 family. [ABSTRACT FROM AUTHOR]

Published

2006

3. IL-22 Increases the Innate Immunity of Tissues

Author

Wolk, Kerstin, Kunz, Stefanie, Witte, Ellen, Friedrich, Markus, Asadullah, Khusru, and Sabat, Robert

Subjects

*INTERLEUKINS, *IMMUNITY, *TISSUES, *T cells

Abstract

Interleukin 22 (IL-22) is mainly produced by activated Th1 cells. The data presented here indicate that neither resting nor activated immune cells express IL-22 receptor, and IL-22 did not have any effects on these cells in vitro and in vivo. In contrast, cells of the skin and the digestive and respiratory systems represent putative targets of this cytokine. The expression of IL-22 receptor in keratinocytes was upregulated by Interferon-γ. In these cells, IL-22 activated STAT3 and directly and transcriptionally increased the expression of β-Defensin 2 and β-Defensin 3. High levels of IL-22 were associated with strongly upregulated β-Defensin expression in skin from patients with T cell-mediated dermatoses. Taken together, IL-22 does not serve the communication between immune cells but is a T cell mediator that directly promotes the innate, nonspecific immunity of tissues. [Copyright &y& Elsevier]

Published

2004

4. Etiology and Long-Term Prognosis of Unilateral Paramedian Pontine Infarction with Progressive Symptoms.

Author

Kunz, Stefanie, Griese, Harald, and Busse, Otto

Subjects

*INFARCTION, *BLOOD circulation disorders, *CEREBROVASCULAR disease, *ETIOLOGY of diseases, *PROGNOSIS

Abstract

Progressive pure motor hemiparesis is a common feature in paramedian pontine infarction. To assess the etiology, clinical course and long-term prognosis of this stroke subtype, we identified 26 patients with progressive symptoms in a retrospective study, treated in our hospital between 1993 and 1998. All patients had more than one stroke risk factor, and in 20, basilar branch disease, an atherosclerotic occlusion of basilar perforating arteries, was causative. Most patients developed severe hemiparesis after a mean time of 3 days, nearly 50% showed deterioration in connection with a fall in systolic blood pressure. The patients were followed up for 4–9 years: 4 patients had further strokes, 5 died, and 17 patients were independent, which may be interpreted as a good long-term prognosis.Copyright © 2003 S. Karger AG, Basel [ABSTRACT FROM AUTHOR]

Published

2003

5. Multiple Mechanisms of Reduced Major Histocompatibility Complex Class II Expression in Endotoxin Tolerance.

Author

Wolk, Kerstin, Kunz, Stefanie, Crompton, Nigel E.A., Volk, Hans-Dieter, and Sabat, Robert

Subjects

*MAJOR histocompatibility complex, *ENDOTOXINS, *MONOCYTES

Abstract

Focuses on the mechanism behind reduced major histocompatibility complex (MHC) class II expression in endotoxin tolerance. Effect of endotoxin priming on monocyte intracellular MHC class II; Reduction of the expression of chaperonic invariant chain; Inhibited synthesis of the major lysosomal enzyme for final cleavage of the invariant chain going along with a relative accumulation of p10.

Published

2003

6. IL-19 Is a Component of the Pathogenetic IL-23/IL-17 Cascade in Psoriasis.

Author

Witte, Ellen, Kokolakis, Georgios, Witte, Katrin, Philipp, Sandra, Doecke, Wolf-Dietrich, Babel, Nina, Wittig, Bianca M, Warszawska, Katarzyna, Kurek, Agata, Erdmann-Keding, Magdalena, Kunz, Stefanie, Asadullah, Khusru, Kadin, Marshall E, Volk, Hans-Dieter, Sterry, Wolfram, Wolk, Kerstin, and Sabat, Robert

Subjects

*PSORIASIS, *CYTOKINES, *KERATINOCYTES, *CHEMOKINES, *TUMOR necrosis factors, *METALLOPROTEINASES, *NEUTROPHILS

Abstract

Psoriasis is a common chronic inflammatory disease with characteristic skin alterations and functions as a model of immune-mediated disorders. Cytokines have a key role in psoriasis pathogenesis. Here, we demonstrated that out of 30 individually quantified cytokines, IL-19 showed the strongest differential expression between psoriatic lesions and healthy skin. Cutaneous IL-19 overproduction was reflected by elevated IL-19 blood levels that correlated with psoriasis severity. Accordingly, anti-psoriatic therapies substantially reduced both cutaneous and systemic IL-19 levels. IL-19 production was induced in keratinocytes by IL-17A and was further amplified by tumor necrosis factor-α and IL-22. Among skin cells, keratinocytes were found to be important targets of IL-19. IL-19 alone, however, regulated only a few keratinocyte functions. While increasing the production of S100A7/8/9 and, to a moderate extent, also IL-1β, IL-20, chemokine C-X-C motif ligand 8, and matrix metalloproteinase 1, IL-19 had no clear influence on the differentiation, proliferation, or migration of these cells. Importantly, IL-19 amplified many IL-17A effects on keratinocytes, including the induction of β-defensins, IL-19, IL-23p19, and T helper type 17-cell- and neutrophil-attracting chemokines. In summary, IL-19 as a component of the IL-23/IL-17 axis strengthens the IL-17A action and might be a biomarker for the activity of this axis in chronic inflammatory disorders. [ABSTRACT FROM AUTHOR]

Published

2014

7. Deficiency of IL-22 Contributes to a Chronic Inflammatory Disease: Pathogenetic Mechanisms in Acne Inversa.

Author

Wolk, Kerstin, Warszawska, Katarzyna, Hoeflich, Conny, Witte, Ellen, Schneider-Burrus, Sylke, Witte, Katrin, Kunz, Stefanie, Buss, Annette, Roewert, Hans Joachim, Krause, Markus, Lukowsky, Ansgar, Volk, Hans-Dieter, Sterry, Wolfram, and Sabat, Robert

Subjects

*T cells, *CYTOKINES, *CARRIER proteins, *SKIN inflammation, *INFLAMMATION, *EPIDERMIS

Abstract

Overexpression of the T cell cytokine IL-22 is linked to the development of some chronic diseases, but little is known about IL-22 deficiency in humans. As demonstrated in this study, acne inversa (AI; also designated as Hidradenitis suppurativa) lesions show a relative deficiency of IL-22 and IL-20, but not of IL-17A, IL-26, IFN-γ, IL-24, or IL-1β. Moreover, AI lesions had reduced expression of membranous IL-22 and IL-20 receptors and increased expression of the natural IL-22 inhibitor, IL-22 binding protein. AI is a chronic inflammatory skin disease with prevalence up to 4% of the population and in which cutaneous bacterial persistence represents an important pathogenetic factor. Accordingly, we also found a relative deficiency of antimicrobial proteins (AMPs) in AI lesions and a positive correlation between lesional IL-22 and IL-20 versus AMP levels. IL-22, like its tissue cell downstream mediator IL-20, upregulated AMPs in reconstituted human epidermis and was critical for increased AMP levels under inflammatory conditions. The relative IL-22 deficiency in AI was not linked to lesional T cell numbers or Th22/Th1/Th17 subset markers and -inducing cytokines. However, IL-10 was highly expressed in AI lesions and correlated negatively with IL-22 expression. Moreover, IL-10 inhibited IL-22 but not IL-17 production in vitro. The IL-10 overexpression, in turn, was not associated with an elevated presence of regulatory T cells but with the enhanced presence of an IL-10-inducing cytokine. We conclude that IL-22 deficiency may contribute to the pathogenesis of certain chronic disorders as postulated in this paper for AI. [ABSTRACT FROM AUTHOR]

Published

2011