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Rescooped by Gilbert C FAURE from Cancer Immunotherapy Review and Collection
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The IL-20 subfamily of cytokines [mdash] from host defence to tissue homeostasis : Nature Reviews Immunology : Nature Publishing Group

The IL-20 subfamily of cytokines [mdash] from host defence to tissue homeostasis : Nature Reviews Immunology : Nature Publishing Group | Immunology | Scoop.it
From www.nature.com - January 1, 2015 1:58 PM
Abstract

The interleukin-20 (IL-20) subfamily of cytokines comprises IL-19, IL-20, IL-22, IL-24 and IL-26. These cytokines are all members of the larger IL-10 family, but have been grouped together to form the IL-20 subfamily based on their usage of common receptor subunits and similarities in their target-cell profiles and biological functions. Members of the IL-20 subfamily facilitate the communication between leukocytes and epithelial cells, thereby enhancing innate defence mechanisms and tissue repair processes at epithelial surfaces. In this Review, we describe the cellular sources and targets of the IL-20 subfamily cytokines, and we detail how their expression is regulated. Much of our understanding of the unique biology of this group of cytokines is still based on IL-22, which is the most studied member of the IL-20 subfamily. Nevertheless, we attempt a broader discussion of the emerging functions of IL-20 subfamily cytokines in host defence, inflammatory diseases, cancer and metabolism.


Via Krishan Maggon
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Krishan Maggon 's curator insight, December 14, 2014 2:22 AM

NATURE REVIEWS IMMUNOLOGY | REVIEW

 The IL-20 subfamily of cytokines — from host defence to tissue homeostasisSascha Rutz,Xiaoting Wang& Wenjun OuyangAffiliationsCorresponding authorNature Reviews Immunology 14, 783–795 (2014) doi:10.1038/nri3766Published online 25 November 2014
Gilbert C FAURE's curator insight, December 14, 2014 4:14 AM

nice review
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Rescooped by Gilbert C FAURE from Cancer Immunotherapy Review and Collection
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STING-Dependent Cytosolic DNA Sensing Mediates Innate Immune Recognition of Immunogenic Tumors: Immunity

From www.cell.com - November 23, 2014 2:24 PM
Highlights

 

•Spontaneous T cell responses against tumors require the host STING pathway in vivo•Tumor-derived DNA can induce type I interferon production via STING•Tumor DNA can be identified in host APCs in the tumor microenvironment in vivo

 

Summary

Spontaneous T cell responses against tumors occur frequently and have prognostic value in patients. The mechanism of innate immune sensing of immunogenic tumors leading to adaptive T cell responses remains undefined, although type I interferons (IFNs) are implicated in this process. We found that spontaneous CD8+T cell priming against tumors was defective in mice lacking stimulator of interferon genes complex (STING), but not other innate signaling pathways, suggesting involvement of a cytosolic DNA sensing pathway. In vitro, IFN-β production and dendritic cell activation were triggered by tumor-cell-derived DNA, via cyclic-GMP-AMP synthase (cGAS), STING, and interferon regulatory factor 3 (IRF3). In the tumor microenvironment in vivo, tumor cell DNA was detected within host antigen-presenting cells, which correlated with STING pathway activation and IFN-β production. Our results demonstrate that a major mechanism for innate immune sensing of cancer occurs via the host STING pathway, with major implications for cancer immunotherapy.


Via Krishan Maggon
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