Your search keyword '"Wolk K"' showing total 21 results

1. Pathogenese der Hidradenitis suppurativa/Acne inversa.

Author

Nikolakis, G., Kokolakis, G., Kaleta, K., Wolk, K., Hunger, R., Sabat, R., and Zouboulis, C. C.

Abstract

Copyright of Der Hautarzt is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2021

2. Activity and components of the granulocyte colony‐stimulating factor pathway in hidradenitis suppurativa*.

Author

Wolk, K., Brembach, T.‐C., Šimaitė, D., Bartnik, E., Cucinotta, S., Pokrywka, A., Irmer, M.L., Triebus, J., Witte‐Händel, E., Salinas, G., Leeuw, T., Volk, H.‐D., Ghoreschi, K., and Sabat, R.

Subjects

GRANULOCYTE-colony stimulating factor, KINASES, BACTERIAL enzymes, MATRIX metalloproteinases, CELL populations, TUMOR necrosis factor receptors, HIDRADENITIS suppurativa

Abstract

Summary: Background: Hidradenitis suppurativa (HS) is a chronic inflammatory disease, characterized by painful, purulent and destructive skin alterations in intertriginous areas. Objectives: We investigated the expression and role in HS of granulocyte colony‐stimulating factor (G‐CSF), the regulator of neutrophil biology, as clinical signs of a neutrophilic granulocyte‐driven inflammation are distinctive in the disease. Methods: Skin and blood samples obtained from different cohorts of patients with HS and control individuals were assessed by RNA sequencing, quantitative polymerase chain reaction on reverse transcribed mRNA, and/or enzyme‐linked immunosorbent assay. Mechanistic studies using keratinocytes, dermal fibroblasts, immune cell populations and skin biopsies were performed. Results: G‐CSF was abundant in HS skin, particularly in inflamed nodules and abscesses. Its levels even exceeded those found in other inflammatory skin diseases. Interleukin (IL)‐1 and IL‐17, respectively, induced G‐CSF production by fibroblasts and keratinocytes. These effects were enhanced by tumour necrosis factor (TNF)‐α and IL‐36. Accordingly, fibroblasts separated from HS lesions expressed G‐CSF, and IL‐1 receptor antagonist reduced G‐CSF levels in explanted HS skin. G‐CSF blood levels positively correlated with severity of HS. Elevated lesional G‐CSF receptor levels were linked to upregulation of molecules that contribute to prolonged activation of neutrophils by components of bacteria and damaged host cells [formyl peptide receptor 1 (FPR1), FPR2 and free fatty acid receptor 2 (FFAR2)], neutrophil survival [TNF receptor superfamily member 10C (TNFRSF10C/TRAIL‐R3) and TNF receptor superfamily member 6B], kinases (tyrosine‐protein kinase HCK and hexokinase 3), and skin destruction [MMP25 (matrix metalloproteinase 25) and ADAM8 (disintegrin and metalloproteinase domain‐containing protein 8)]. G‐CSF elevated the expression of FPR1, FFAR2, and TNFRSF10C/TRAIL‐R3 in neutrophils and synergized with bacterial components to induce skin‐destructive enzymes. Conclusions: The G‐CSF pathway engages both tissue and immune cells, is strongly activated in HS lesions, and offers the opportunity to target the neutrophil‐driven inflammation. What is already known about this topic? Hidradenitis suppurativa (HS) is a chronic debilitating skin disorder with a very high, unmet medical need.The diseased skin in patients with HS shows distinct features of a neutrophil‐driven inflammation (e.g. abscess formation, purulent discharge).Granulocyte colony‐stimulating factor (G‐CSF) is the major regulator of neutrophil development, survival and function. What does this study add? HS lesions show highly increased levels of G‐CSF and its receptor.Major G‐CSF inducers are interleukin (IL)‐1β and IL‐17.In neutrophils, G‐CSF upregulates receptors for components of bacteria and damaged host cells, decoy receptors for apoptosis inducers and proteases.The production of skin‐destructive enzymes induced by bacterial components is strengthened by G‐CSF in neutrophils.G‐CSF inducers and molecules upregulated by G‐CSF in neutrophils in vitro are abundant in HS lesions. What is the translational message? G‐CSF is the central element of a pathogenetic pathway in HS.The G‐CSF pathway may contribute to the persistence of abscesses, purulent secretion and progressive skin structure destruction.Targeting G‐CSF or its pathway elements may represent an approach for the treatment of HS and other conditions with neutrophil‐driven inflammation and skin destruction. Linked Comment: E.J. Giamarellos‐Bourboulis. Br J Dermatol 2021; 185:15–16. [ABSTRACT FROM AUTHOR]

Published

2021

3. Aetiology and pathogenesis of hidradenitis suppurativa.

Author

Wolk, K., Join‐Lambert, O., and Sabat, R.

Subjects

HIDRADENITIS suppurativa, ETIOLOGY of diseases, T helper cells, SUPPRESSOR cells, GENETICS

Abstract

Summary: Hidradenitis suppurativa (HS) is a chronic inflammatory disorder. Patients develop inflamed nodules and abscesses and, at later stages of disease, epithelialized tunnels and scars in skinfolds of axillary, inguinal, gluteal and perianal areas. Quality of life is affected due to severe pain, purulent secretion, restricted mobility and systemic involvement. Genetics and lifestyle factors including smoking and obesity contribute to the development of HS. These factors lead to microbiome alteration, subclinical inflammation around the terminal hair follicles, and infundibular hyperkeratosis, resulting in plugging and rupture of the follicles. Cell‐damage‐associated molecules and propagating bacteria trigger inflammation and lead to massive immune cell infiltration that clinically manifests as inflamed nodules and abscesses. The immune system plays a key role also in the progression and chronification of skin alterations. Innate proinflammatory cytokines (e.g. interleukin‐1β and tumour necrosis factor‐α), mediators of activated T helper (Th)1 and Th17 cells (e.g. interleukin‐17 and interferon‐γ), and effector mechanisms of neutrophilic granulocytes, macrophages and plasma cells are involved. Simultaneously, skin lesions contain anti‐inflammatory mediators (e.g. interleukin‐10) and show limited activity of Th22 and regulatory T cells. The inflammatory vicious circle finally results in pain, purulence, tissue destruction and scarring. Chronic inflammation in patients with HS is also frequently detected in organs other than the skin, as indicated by their comorbidities. All these aspects represent a challenge for the development of therapeutic approaches, which are urgently needed for this debilitating disease. This scholarly review focuses on the causes and pathogenetic mechanisms of HS and the potential therapeutic value of this knowledge. [ABSTRACT FROM AUTHOR]

Published

2020

4. Association of CCL2 with systemic inflammation in Schnitzler syndrome.

Author

Krause, K., Sabat, R., Witte‐Händel, E., Schulze, A., Puhl, V., Maurer, M., and Wolk, K.

Subjects

MONOCLONAL gammopathies, DISEASE duration, HIDRADENITIS suppurativa, ENZYME-linked immunosorbent assay, EPITHELIAL cells, POLYMERASE chain reaction, INFLAMMATORY mediators

Abstract

Summary: Background: Schnitzler syndrome (SchS) is a rare autoinflammatory disease characterized by urticarial exanthema, bone and joint alterations, fever and monoclonal gammopathy, which manifest mostly in the second half of life. It involves overactivation of the interleukin (IL)‐1 system, but the exact pathophysiological pathways remain largely unknown. Objectives: To identify and characterize the pathogenetic players in SchS. Methods: Blood parameters were quantified in patients with SchS compared with healthy controls and patients with psoriasis and hidradenitis suppurativa using enzyme‐linked immunosorbent assay (ELISA). CCL2 expression in cultured primary cells was analysed by quantitative reverse‐transcriptase polymerase chain reaction and ELISA. Results: CCL2, a chemoattractant for monocytic and further mononuclear immune cells, was found to be significantly elevated in patients with SchS. CCL2 levels showed a positive association with global disease activity, especially with bone pain, but not disease duration, gammopathy, neutrophilia or skin disease. In vitro stimulation assays demonstrated a strong CCL2 production capacity of mononuclear immune cells and fibroblasts, but not epithelial or endothelial cells. Among a range of inflammatory mediators, only IL‐1β (immune cells, fibroblasts) and tumour necrosis factor (TNF)‐α (fibroblasts) were important CCL2 inducers. TNF‐α, but not IL‐17, strengthened the CCL2‐inducing effect of IL‐1β in fibroblasts. Accordingly, CCL2 levels positively correlated with both TNF‐α and IL‐1β serum levels in patients with SchS. Therapeutic IL‐1β blockade decreased CCL2 blood levels in these patients as early as 1 week after the initiation of treatment. Conclusions: CCL2 may be an important component of the pathogenetic cascade leading to bone alterations, and a suitable marker of disease activity in patients with SchS. What's already known about this topic?Schnitzler syndrome (SchS) is a very rare acquired autoinflammatory disease, clinically characterized by urticarial exanthema, arthralgia and osteosclerosis, and episodes of fever.The pathogenesis involves overactivation of the interleukin‐1 system.The exact pathogenetic pathways are mostly unknown, and biomarkers are not available to assess the inflammatory activity in SchS. What does this study add? The chemokine CCL2 is a marker of SchS; its blood levels are significantly upregulated and linked to global disease activity and early therapy response in patients with SchS.While no clear relationship with patients' urticarial exanthema was detected, CCL2 may be involved in bone alterations in these patients.The cellular sources of CCL2 include mononuclear immune cells and fibroblasts.Interleukin‐1β and tumour necrosis factor‐α, blood levels of which correlate with CCL2 levels in patients with SchS, are important CCL2 inducers. What is the translational message? Quantifying CCL2 blood levels may allow the objective estimation of inflammatory disease activity and may help with the therapy decision in patients with SchS.CCL2 may be a key element of the pathogenetic cascades in SchS, especially those important for osteosclerosis. Linked Comment:Kambe and Nguyen. Br J Dermatol 2019; 180:706–707. Respond to this article Plain language summary available online [ABSTRACT FROM AUTHOR]

Published

2019

5. Absence of specific alternatively spliced exon of CD44 in macrophages prevents colitis.

Author

Wittig, B M, Sabat, R, Holzlöhner, P, Witte-Händel, E, Heilmann, K, Witte, K, Triebus, J, Tzankov, A, Laman, J D, Bokemeyer, B, Terracciano, L, Schwärzler, C, Kohler, H, Volkmer, R, Loddenkemper, C, Wolk, K, Hoffmann, U, and Günthert, U

Published

2018

6. Acne inversa/Hidradenitis suppurativa: Ein Update.

Author

Sabat, R., Tsaousi, A., Rossbacher, J., Kurzen, H., Fadai, T., Schwichtenberg, U., Schneider-Burrus, S., Kokolakis, G., and Wolk, K.

Abstract

Copyright of Der Hautarzt is the property of Springer Nature and its content may not be copied or emailed to multiple sites or posted to a listserv without the copyright holder's express written permission. However, users may print, download, or email articles for individual use. This abstract may be abridged. No warranty is given about the accuracy of the copy. Users should refer to the original published version of the material for the full abstract. (Copyright applies to all Abstracts.)

Published

2017

7. Lipocalin-2 is expressed by activated granulocytes and keratinocytes in affected skin and reflects disease activity in acne inversa/hidradenitis suppurativa.

Author

Wolk, K., Wenzel, J., Tsaousi, A., Witte ‐ Händel, E., Babel, N., Zelenak, C., Volk, H. ‐ D., Sterry, W., Schneider ‐ Burrus, S., and Sabat, R.

Subjects

LIPOCALINS, GRANULOCYTES, KERATINOCYTES, HIDRADENITIS suppurativa, SKIN diseases

Abstract

Background Acne inversa ( AI)/hidradenitis suppurativa is a chronic inflammatory disease characterized by painful axillary, inguinal and perianal skin lesions with deep-seated nodules, abscesses and fistulae. Objectives This study aimed to identify and characterize the key players in AI pathogenesis. Methods Epidemiological and anamnestic data for patients with AI were collected, and blood and skin samples were also taken. Healthy participants and patients with psoriasis served as controls. Assessment of samples and cultures of primary cells was performed by enzyme-linked immunosorbent assay, quantitative polymerase chain reaction on reverse transcribed mRNA, and immunohistochemistry. Results Of 35 mediators quantified in the blood of patients with AI, lipocalin-2 ( LCN2) appeared as one of the most significantly upregulated parameters compared with healthy participants [85·8 ± 12·2 ( n = 18) vs. 41·8 ± 4·2 ( n = 15); P < 0·001]. Strongly elevated LCN2 expression was present in AI lesions, with granulocytes and keratinocytes being sources of this expression. In vitro, these cells upregulated LCN2 production in response to tumour necrosis factor ( TNF)-α, and a positive relationship between systemic TNF-α and LCN2 levels ( rs = 0·55, P = 0·011; n = 20) was evident for AI. LCN2 blood levels correlated with AI disease severity ( rs = 0·65, P < 0·001; n = 29), but not with disease duration, age, sex, body mass index or smoking habit. Detailed analyses revealed a link with the number of skin regions containing nodules and fistulae, but not scars. Conclusions LCN2 might serve as a blood biomarker for the objective assessment of inflammatory activity in AI. We suggest a self-amplification loop comprising TNF-α, neutrophilic granulocytes and LCN2, which contributes to the recurrent skin neutrophil infiltration in AI, clinically evident as pus. [ABSTRACT FROM AUTHOR]

Published

2017

8. Interleukin-10 receptor-1 expression in monocyte-derived antigen-presenting cell populations: dendritic cells partially escape from IL-10's inhibitory mechanisms.

Author

von Lanzenauer, S H, Wolk, K, Höflich, C, Kunz, S, Grünberg, B H, Döcke, W-D, Reineke, U, Asadullah, K, Sterry, W, Volk, H-D, and Sabat, R

Subjects

INTERLEUKIN-10, IMMUNOMODULATORS, MONOCYTES, MACROPHAGES, MYELOID leukemia, LEUKEMIA treatment

Abstract

Interleukin (IL)-10 is an important immunoregulatory cytokine that mediates its effects via a transmembrane receptor complex consisting of two different chains, IL-10R1 and IL-10R2. While IL-10R2 is ubiquitously expressed and does not bind IL-10 primarily, the expression of IL-10R1 determines cellular responsiveness. However, the current knowledge about the expression and regulation of IL-10R1 is still limited. Here we analyzed the expression of IL-10R1 on monocytic cells and demonstrated that human blood monocytes carried about 720 IL-10-binding sites on their surface. Compared with lymphocytes and various tissue cells and tissues, blood monocytes expressed the highest IL-10R1 levels. The in vitro differentiation of these cells into macrophages provoked a further increase of IL-10R1 surface expression. In contrast, their differentiation into myeloid dendritic cells (mDCs) resulted in reduced surface IL-10R1 levels. The different IL-10R1 levels expressed by monocyte-derived antigen-presenting cell populations were reflected in their different responsiveness toward IL-10. Importantly, also in vivo developed immature macrophages and mDCs showed different IL-10 sensitivity. These data suggest that, compared with monocytes and macrophages, mDCs partially escape from IL-10's inhibitory mechanisms by downregulating IL-10R1. [ABSTRACT FROM AUTHOR]

Published

2015

9. Multisystem Cranial Polyneuritis and Ganglionitis in a Dog.

Author

Foss, K., da Costa, R.C., Wolk, K., Stromberg, P., Guo, L.T., and Shelton, G.D.

Subjects

CASE studies, GOLDEN retriever, DOG diseases, POLYNEURITIS, CRANIAL nerves, JAWS

Abstract

The article describes the case of a four-year-old spayed-female Golden Retriever which was diagnosed with multisystem cranial polyneuritis and ganglionitis. The dog had a history of difficulty closing the jaw. The clinical findings showed a dysfunction of the sensory, autonomic, and motor components of several cranial nerves.

Published

2011

10. Despite IFN-λ receptor expression, blood immune cells, but not keratinocytes or melanocytes, have an impaired response to type III interferons: implications for therapeutic applications of these cytokines.

Author

Witte, K., Gruetz, G., Volk, H.-D., Looman, A. C., Asadullah, K., Sterry, W., Sabat, R., and Wolk, K.

Subjects

CELLULAR immunity, IMMUNOREGULATION, EPITHELIAL cells, ANTINEOPLASTIC agents, KERATINOCYTES

Abstract

Interferon (IFN)-λ1, -2 and -3 (also designated as interleukin (IL)-29, IL-28α and IL-28β) represent a new subfamily within the class II cytokine family. They show type I IFN-like antiviral and cytostatic activities in affected cells forming the basis for IFN-λ1 therapy currently under development for hepatitis C infection. However, many aspects of IFN-λs are still unknown. This study aimed at identifying the target cells of IFN-λs within the immune system and the skin. Among skin cell populations, keratinocytes and melanocytes, but not fibroblasts, endothelial cells or subcutaneous adipocytes turned out to be targets. In contrast to these target cells, blood immune cell populations did not clearly respond to even high concentrations of these cytokines, despite an IFN-λ receptor expression. Interestingly, immune cells expressed high levels of a short IFN-λ receptor splice variant (sIFN-λR1/sIL-28R1). Its characterization revealed a secreted, glycosylated protein that binds IFN-λ1 with a moderate affinity (KD 73 nM) and was able to inhibit IFN-λ1 effects. Our study suggests that IFN-λ therapy should be suited for patients with verrucae, melanomas and non-melanoma skin cancers, apart from patients with viral hepatitis, and would not be accompanied by immune-mediated complications known from type I IFN application. [ABSTRACT FROM AUTHOR]

Published

2009

11. Long-term interleukin-10 presence induces the development of a novel, monocyte-derived cell type.

Author

Schoenbein, C., Docke, W.-D., Wolk, K., Belbe, G., Hoflich, C., Jung, M., Grutz, G., Sterry, W., Volk, H.-D., Asadullah, K., and Sabat, R.

Subjects

IMMUNOREGULATION, TUMOR necrosis factors, CELLULAR immunity, VIRUS diseases, CLINICAL trials, THERAPEUTICS, IMMUNOLOGY

Abstract

Interleukin (IL)-10 is one of the most crucial immunoregulatory cytokines. Its short-term effects have been analysed extensively, but little is known about its long-term effects. This is of considerable importance, as high systemic IL-10 levels are present for long periods in patients with persistent viral infections, certain cancers and in critical care patients. Our study investigated the effects of the long-term presence of IL-10 on human peripheral blood monocytes. In vitro, IL-10 treatment of these cells for 7 days induced the development of a novel cell type characterized by unique phenotypical and functional characteristics. These cells showed high HLA-DR expression and low expression of CD86 and other co-stimulatory molecules on their surface. The mRNA levels of both HLA-DR and CD86 were high, but no intracellular accumulation of CD86 protein was observed. With respect to its function, these cells showed strongly diminished tumour necrosis factor-α production following lipopolysaccharide stimulation, strongly diminished allogenic CD4+ T cell stimulatory capacity, and even induced a hyporesponsive state in CD4+ T cells. The phenotype remained stable despite the removal of IL-10. In vivo, we found monocytic cells from patients exhibiting this phenotype after long-term IL-10 exposure. These results complement our knowledge further about the biological effects of IL-10 and may provide an explanation for the sustained immunodeficiency in cases of the persistent presence of systemic IL-10. [ABSTRACT FROM AUTHOR]

Published

2008

12. Reduced monocyte CD86 expression in postinflammatory immunodeficiency.

Author

Wolk K, Höflich C, Zuckermann-Becker H, Döcke W, Volk H, and Sabat R

Published

2007

13. The expression of legumain, an asparaginyl endopeptidase that controls antigen processing, is reduced in endotoxin-tolerant monocytes.

Author

Wolk, K., Grütz, G., Witte, K., Volk, H.-D., and Sabat, R.

Subjects

MONOCYTES, ENDOTOXINS, ENDOPEPTIDASES, ANTIGENS, B cells

Abstract

The exposition of monocytes to lipopolysaccharide (LPS) primarily causes a massive inflammatory response that is then followed by a hyporesponsive state of these cells. This latter state is called endotoxin tolerance and is characterized by (i) the attenuated production of proinflammatory mediators after repeated LPS treatment, and (ii) the diminished antigen presentation and T-cell stimulation capacity. The data presented here indicate that LPS priming causes a specific decrease in the expression of legumain (the asparaginyl endopeptidase responsible for the key step in antigen processing) in monocytes. In these cells, the fraction of major histocompatibility complex (MHC) class II loaded with CLIP was increased. In contrast to monocytes, LPS priming provoked an increase of legumain expression in B cells. Reduced monocytic expression of legumain was also found in critically ill patients supporting the suitability of endotoxin tolerance as an experimental model of clinical postinflammatory immunodeficiency.Genes and Immunity (2005) 6, 452–456. doi:10.1038/sj.gene.6364224; published online 5 May 2005 [ABSTRACT FROM AUTHOR]

Published

2005

14. Association of diet with serum insulin-like growth factor I in middle-aged and elderly men.

Author

Larsson SC, Wolk K, Brismar K, and Wolk A

Abstract

BACKGROUND: Insulin-like growth factor I (IGF-I) has been implicated in several chronic diseases, including cancer, heart disease, and osteoporosis. OBJECTIVE: Our aim was to assess whether intakes of total energy, alcohol, vitamins, minerals, and foods rich in protein and minerals (including red meat, fish and seafood, poultry, and milk) are associated with serum IGF-I concentrations in middle-aged and elderly men. DESIGN: We measured serum IGF-I concentrations in 226 free-living healthy men aged 42-76 y. The average of fourteen 24-h dietary telephone interviews performed over 1 y was used to estimate long-term dietary intake. RESULTS: We observed statistically significant positive associations between intakes of protein (P for trend = 0.001) and zinc (P for trend = 0.002) and serum IGF-I concentrations after adjusting for age. The difference in mean IGF-I concentrations for the highest compared with the lowest quintile of intake was approximately 17% (162 microg/L compared with 139 microg/L) for protein and approximately 16% (166 microg/L compared with 143 microg/L) for zinc. Consumption of red meat (P for trend = 0.05) and fish and seafood (P for trend = 0.07) was modestly positively associated with IGF-I concentrations. Other dietary factors were not associated with IGF-I concentrations. CONCLUSION: In this population of healthy well-nourished men, greater dietary intakes of protein, zinc, red meat, and fish and seafood were associated with higher IGF-I concentrations. Copyright © 2005 American Society for Clinical Nutrition [ABSTRACT FROM AUTHOR]

Published

2005

15. Is there an interaction between interleukin-10 and interleukin-22?

Author

Wolk, K, Witte, E, Reineke, U, Witte, K, Friedrich, M, Sterry, W, Asadullah, K, Volk, H-D, and Sabat, R

Subjects

INTERLEUKIN-10, CYTOKINES, RETICULO-endothelial system, CELLULAR immunity, PEPTIDES, IMMUNOREGULATION

Abstract

Interleukin(IL)-10 and IL-22 are structurally related cytokines. Their heterodimeric receptors consist of the cytokine-specific chains IL-10R1 and IL-22R1, respectively, and the common chain IL-10R2. This study focused on the question of whether IL-10 modulates IL-22 effects and vice versa. This question is important because IL-10 and IL-22 exert anti- and proinflammatory effects, respectively, and, as we show here, are simultaneously present in both systemic and local inflammation. The revealed lacking concomitance of IL-10R1 and IL-22R1 on identical cells excluded any possible interaction between IL-10 and IL-22 apart from the competition for IL-10R2. To study this competition, monocytes and hepatocytes were chosen. The dependence of the cytokine action on IL-10R2 was verified. Interestingly, no influence of IL-22 on IL-10 effects was observed. The same was true when IL-22 was used in complex with IL-22-binding protein. Similarly, no influence of IL-10 was found on IL-22 action. This missing competition seemed to be due to a lack of binding between IL-10R2 and the native cytokines in the absence of their corresponding R1 chain. However, IL-10R2 interacted with defined IL-10- and IL-22-derived peptides supporting the hypothesis that cytokine binding to its corresponding R1 chain creates a binding site on this cytokine for IL-10R2.Genes and Immunity (2005) 6, 8-18. doi:10.1038/sj.gene.6364144 Published online 4 November 2004 [ABSTRACT FROM AUTHOR]

Published

2005

16. Cloning of murine IL-22 receptor alpha 2 and comparison with its human counterpart.

Author

Weiss, B., Wolk, K., Grünberg, B. H., Volk, H.-D., Sterry, W., Asadullah, K., and Sabat, R.

Subjects

INTERLEUKINS, GENE expression, INTERFERONS, CHROMOSOMES, MESSENGER RNA, INFLAMMATION, IMMUNITY

Abstract

We have identified the mouse and rat homologs of human interleukin-22 receptor alpha 2 (IL-22Ra2) and compared the localization, structure, and expression of the encoding murine and human genes. The mouse IL-22Ra2-encoding gene is located on chromosome 10A3 between, like in human, the genes for interferon-gamma R1 and IL-20R1. It spans a region of approximately 10?kb therefore being three times shorter than the human gene. Although the overall gene structure in both species is similar, the mouse gene lacks a counterpart to the third coding exon of the human gene known to be alternatively spliced. Like in human, mouse and rat IL-22Ra2 exist only as soluble receptors as deduced from the lack of transmembrane and intracellular domains encoding sequences. Quantitative expression analyses showed, analogically to the human system, a limited tissue distribution of mouse IL-22Ra2 mRNA. Differential modulation of IL-22Ra2 mRNA expression was observed upon systemic inflammation in mice in spleen, thymus, and lymph node.Genes and Immunity (2004) 5, 330-336. doi:10.1038/sj.gene.6364104 Published online 17 June 2004 [ABSTRACT FROM AUTHOR]

Published

2004

17. A novel, soluble homologue of the human IL-10 receptor with preferential expression in placenta.

Author

Gruenberg, B H, Schoenemeyer, A, Weiss, B, Toschi, L, Kunz, S, Wolk, K, Asadullah, K, and Sabat, R

Subjects

CELL receptors, CYTOKINES, MESSENGER RNA, GENE expression

Abstract

The cytokine receptor family type 2 (CRF2) comprises receptors for important immunomediators like interferons and interleukin-10 (IL-10). We identified a novel member of this family which represents the first exclusively soluble receptor in this group and was therefore designated as CRF2-soluble 1 (CRF2-s1). The CRF2-s1 gene covers about 28 kb and is located on chromosome 6 in close proximity to the CRF2 members interferon (IFN)-γ receptor 1 and IL-20 receptor 1. It comprises seven exons and generates two different mRNA splice variants, CRF2-s1-long and CRF2-s1-short. CRF2-s1-long and CRF2-s1-short encode proteins of 263 and 231 amino acids, respectively. A comparison of predicted protein structures led to the postulation that each receptor variants binds a different ligand. Quantitative analysis of human mRNA expression revealed a very restricted pattern for both splice forms. CRF2-s1 turned out to be the first member of this receptor family which was expressed neither in resting nor in stimulated leucocyte populations. CRF2-s1-long was only expressed in placenta, whereas CRF2-s1-short was additionally expressed in human mammary gland and, at a lower level, in skin, spleen, thymus and stomach. The preferential expression of CRF2-s1 in placenta suggests a role for this receptor in establishing and maintaining successful pregnancy. Genes and Immunity (2001) 2, 329–334. [ABSTRACT FROM AUTHOR]

Published

2001

18. Computer-based detection of depression and dementia in spontaneous speech.

Author

Chlasta, K., Holas, P., and Wolk, K.

Subjects

SPEECH, ARTIFICIAL neural networks, DEMENTIA, MENTAL depression, MENTAL illness, ANXIETY disorders

Abstract

Introduction: There is a significant relation between old-age depression and subsequent dementia in patients aged 50. This supports the hypothesis of old-age depression being a predictor, and possibly a causal factor, of subsequent dementia. The number of people aged 60 years and over has tripled since 1950, reaching 16% in 2050, leading to new medical challenges. Depression is the most common mental disorder in older adults, affecting 7%of the older population. Dementia is the second most common with about 5% prevalence worldwide, but it is the first leading cause of disease burden. Objectives: Early detection and treatment is essential in promoting remission, preventing relapse, and reducing emotional burden. Speech is a well established early indicator of cognitive deficits. Speech processing methods offer great potential to fully automatically screen for prototypic indicators of both dementia and depressive disorders. Methods: We present two different methods to detect pathological speech with artificial neural networks. We use both deep architectures, as well as more traditional machine learning approaches. Results: The models developed using a two-stage deep architecture achieved 59% classification accuracy on the test set from DementiaBank. Our CNN system achieved the best classification accuracy of 63.6% for dementia, but reaching 70% for depressive disorders on the test set from Distress Analysis Interview Corpus. Conclusions: These methods offer a promising classification accuracy ranging from 63% to 70%, applicable in an innovative speechbased screening system. [ABSTRACT FROM AUTHOR]

Published

2021

19. Schnitzler 综合征与 CCL2.

Author

Krause, K., Sabat, R., Witte‐Händel, E., Schulze, A., Puhl, V., Maurer, M., and Wolk, K.

Abstract

Linked Article: Krause et al. Br J Dermatol 2019; 180:859–868 [ABSTRACT FROM AUTHOR]

Published

2019

20. CCL2 in Schnitzler syndrome.

Author

Krause, K., Sabat, R., Witte‐Händel, E., Schulze, A., Puhl, V., Maurer, M., and Wolk, K.

Subjects

CONNECTIVE tissue cells, SYNDROMES, OSTEITIS, RARE diseases

Abstract

Summary: Schnitzler syndrome is a very rare chronic disease, which usually develops in the second half of life. It appears as skin rashes, muscle/skeletal pain and fever episodes. The trigger and molecular processes in the disease are not understood. However, drugs that inhibit the inflammatory molecule called interleukin‐1ß were found to relieve the disease. The authors of this German study wondered which further molecules are involved in Schnitzler syndrome. For this purpose, a range of molecules with inflammatory properties was quantified in the blood of the patients and, as a comparison, in healthy people and patients with other inflammatory diseases. Patients with Schnitzler syndrome were found to have strongly elevated levels of CCL2, a molecule known to attract inflammatory cells to affected tissues and to have a special role in bone alterations. CCL2 levels were particularly high in severely affected patients, especially those with intense bone pain. In the bone, CCL2 is known to be produced by certain bone‐modifying cells. Laboratory experiments revealed that CCL2 was also highly produced by immune cells and connective tissue cells (fibroblasts). Interleukin‐1ß as well as the inflammatory molecule TNF‐α triggered the production of CCL2 by these cells. When patients were treated with an interleukin‐1ß‐blocking drug, health improvement was paralleled by a drop of CCL2 levels. The authors concluded that in Schnitzler syndrome CCL2 is an important player in the inflammation process in bones and other body sites and may be used in the clinic as an indicator of disease severity. Linked Article: Krause et al. Br J Dermatol 2019; 180:859–868 [ABSTRACT FROM AUTHOR]

Published

2019

21. Interleukin-10 receptor-1 expression in monocyte-derived antigen-presenting cell populations: dendritic cells partially escape from IL-10's inhibitory mechanisms.

Author

von Haehling, S, Wolk, K, Höflich, C, Kunz, S, Grünberg, B H, Döcke, W-D, Reineke, U, Asadullah, K, Sterry, W, Volk, H-D, and Sabat, R

Subjects

INTERLEUKIN-10 receptors, GENE expression, MONOCYTES, ANTIGEN presenting cells, DENDRITIC cells, CELL populations

Published

2015