IL-19 and IL-20: two novel cytokines with importance in inflammatory diseases

Sabat, Robert; Wallace, Elizabeth; Endesfelder, Stefanie; Wolk, Kerstin

doi:10.1517/14728222.11.5.601

Cited by 98 publications

(70 citation statements)

References 59 publications

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“…IL-22 and IL-20, although produced by different cell types (IL-22 as a T and NK cell cytokine, and IL-20 being produced by activated keratinocytes and dendritic cells) are two structurally and functionally related cytokines (28,29). The receptor complexes of both cytokines are known to be highly expressed in keratinocytes and are each composed of two different subunits: IL-22R1/IL-10R2 (receptor complex for IL-22), IL-20R1/IL-20R2 (receptor complex I for IL-20), and IL-22R1/IL-20R2 (receptor complex II for IL-20) (28,29).…”

Section: Ai Lesions Show Reduced Upregulation Of Il-22 and Il-20 Exprmentioning

confidence: 99%

“…The receptor complexes of both cytokines are known to be highly expressed in keratinocytes and are each composed of two different subunits: IL-22R1/IL-10R2 (receptor complex for IL-22), IL-20R1/IL-20R2 (receptor complex I for IL-20), and IL-22R1/IL-20R2 (receptor complex II for IL-20) (28,29). For IL-22, there is also a soluble, single-chain receptor called IL-22BP that acts as a high-affinity inhibitor of IL-22 activity (30)(31)(32)(33)(34).…”

Section: Ai Lesions Show Reduced Upregulation Of Il-22 and Il-20 Exprmentioning

confidence: 99%

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

Wolk

Warszawska

Hoeflich

et al. 2011

The Journal of Immunology

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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.

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Section: Ai Lesions Show Reduced Upregulation Of Il-22 and Il-20 Exprmentioning

confidence: 99%

Section: Ai Lesions Show Reduced Upregulation Of Il-22 and Il-20 Exprmentioning

confidence: 99%

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

Wolk

Warszawska

Hoeflich

et al. 2011

The Journal of Immunology

Self Cite

227

283

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“…1,2 The aminoacid sequences of IFN-l2 and IFN-l3 are virtually identical (94%), those of IFN-l2 and IFN-l1 share 66%. These mediators are part of a larger family of structurally related cytokines called the class II cytokine family, which also contains the IL-10-related cytokines (IL-10, IL-19, IL-20, IL-22, IL-24 and IL-26), type I IFNs and IFN-g. [3][4][5] Within the class II cytokine family, IFN-ls form a theoretical bridge between IL-10-related cytokines on the one side and type I IFNs on the other, because they are closer to the first in terms of the structure of their encoding genes, their spatial protein structure and their receptor usage, but their activities mimic many functional aspects of type I IFNs. 1,2,[6][7][8] All three cytokines share the same receptor complex that consists of IFN-lR1 (also designated as IL-28R1) and IL-10R2, 1,2 with IL-10R2 also being part of the receptor complexes for IL-10, IL-22 and IL-26.…”

Section: Introductionmentioning

confidence: 99%

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

et al. 2009

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Interferon (IFN)-l1, -2 and -3 (also designated as interleukin (IL)-29, IL-28a and IL-28b) 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-l1 therapy currently under development for hepatitis C infection. However, many aspects of IFN-ls are still unknown. This study aimed at identifying the target cells of IFN-ls 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-l receptor expression. Interestingly, immune cells expressed high levels of a short IFN-l receptor splice variant (sIFN-lR1/sIL-28R1). Its characterization revealed a secreted, glycosylated protein that binds IFN-l1 with a moderate affinity (K D 73 nM) and was able to inhibit IFN-l1 effects. Our study suggests that IFN-l 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.

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“…Furthermore, the possibility of extending the haplotypic description to neighbouring genes, such as IL-19 should be considered, because skin tissues seem to represent a major target for IL-10-related cytokines, such as IL-19, IL-20, IL-22 and IL-24. [35][36][37] A multivariate analysis of the haplotypes was carried out in relation to skin type and number of nevi adjusted for multiple testing. The haplotypes are based on the gene variations IL-10À7400InDel, IL-10 À6752AT , IL-10 À3538AT , IL-10 À1087GA and IL-10 À597CA .…”

Section: Haplotype Analysismentioning

confidence: 99%

Distal and proximal interleukin (IL)-10 promoter polymorphisms associated with risk of cutaneous melanoma development: a case–control study

Schoof

Bonin

König³

et al. 2009

Genes Immun

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IL-19 and IL-20: two novel cytokines with importance in inflammatory diseases

Cited by 98 publications

References 59 publications

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

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

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

Distal and proximal interleukin (IL)-10 promoter polymorphisms associated with risk of cutaneous melanoma development: a case–control study

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