The signaling suppressor CIS controls proallergic T cell development and allergic airway inflammation

Yang, Xuexian O.; Zhang, Huiyuan; Kim, Byung Seok; Niu, Xiaoyin; Peng, Juan; Chen, Yuhong; Kerketta, Romica; Lee, Young Hee; Chang, Seon Hee; Corry, David B.; Wang, Demin; Watowich, Stephanie S.; Dong, Chen

doi:10.1038/ni.2633

Cited by 115 publications

(125 citation statements)

References 69 publications

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“…Therefore, the level of pSTAT3 in monocytes likely reflects the sum of diverse inflammatory stimuli targeting STAT3. Consistent with these observations, the phosphorylation levels of STAT3 and other STAT proteins have been found to be increased in asthma (30) and in other inflammatory conditions (31). With respect to the influenza vaccine response, our results indicate that the natural variation in circulating free testosterone could drive many of the differences observed in the response to vaccines.…”

Section: Discussionsupporting

confidence: 76%

Systems analysis of sex differences reveals an immunosuppressive role for testosterone in the response to influenza vaccination

Furman

Hejblum

Simon

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

562

501

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Females have generally more robust immune responses than males for reasons that are not well-understood. Here we used a systems analysis to investigate these differences by analyzing the neutralizing antibody response to a trivalent inactivated seasonal influenza vaccine (TIV) and a large number of immune system components, including serum cytokines and chemokines, blood cell subset frequencies, genome-wide gene expression, and cellular responses to diverse in vitro stimuli, in 53 females and 34 males of different ages. We found elevated antibody responses to TIV and expression of inflammatory cytokines in the serum of females compared with males regardless of age. This inflammatory profile correlated with the levels of phosphorylated STAT3 proteins in monocytes but not with the serological response to the vaccine. In contrast, using a machine learning approach, we identified a cluster of genes involved in lipid biosynthesis and previously shown to be up-regulated by testosterone that correlated with poor virus-neutralizing activity in men. Moreover, men with elevated serum testosterone levels and associated gene signatures exhibited the lowest antibody responses to TIV. These results demonstrate a strong association between androgens and genes involved in lipid metabolism, suggesting that these could be important drivers of the differences in immune responses between males and females.

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Section: Discussionsupporting

confidence: 76%

Systems analysis of sex differences reveals an immunosuppressive role for testosterone in the response to influenza vaccination

Furman

Hejblum

Simon

et al. 2013

Proc. Natl. Acad. Sci. U.S.A.

562

501

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“…In particular, skin inflammation is strongly regulated by SOCS1 and SOCS3, as SOCS3 deficiency in keratinocytes causes severe skin inflammation, whereas keratinocyte-specific SOCS1 overexpression down-regulates the expression of specific pro-inflammatory mediators in the skin (30). In the context of type 2 inflammation, the SOCS family member cytokine-inducible SH2-containing protein (CIS) has recently been shown to regulate pro-allergic T helper cell development and to control allergic inflammation (31). In this study, we demonstrated that IL-31 is able to enhance the expression of SOCS1, SOCS2, SOCS3, and CISH in a time-dependent manner.…”

Section: Discussionmentioning

confidence: 99%

Prerequisites for Functional Interleukin 31 Signaling and Its Feedback Regulation by Suppressor of Cytokine Signaling 3 (SOCS3)

Maier

Mittermeir

Ess

et al. 2015

Journal of Biological Chemistry

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Background: Signaling by IL-31 involves OSMR␤ and IL-31R␣, which is expressed in different isoforms. Results: Four of five membrane-bound isoforms activate IL-31 signaling, which is counter-regulated by SOCS3. Conclusion: IL-31 responsiveness is controlled by the expression of specific IL-31R␣ isoforms and is negatively regulated by SOCS proteins. Significance: This study provides new insights into the regulation of IL-31 signaling.

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“…SOCS proteins then provide feedback inhibition by binding to cytokine receptors and JAK kinases. Accordingly, mutations of SOCS1 (100-102) and SOCS3 (103-105) have major effects on erythropoiesis, the immune system, and the placenta, while CISH deletion also affects immunity but in a more subtle way (106).…”

Section: Cell Regulation By Socs-crl5 Complexes and By Socs Proteins mentioning

confidence: 99%

Cell Regulation by Phosphotyrosine-Targeted Ubiquitin Ligases

Cooper

Kaneko

2015

Molecular and Cellular Biology

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Three classes of E3 ubiquitin ligases, members of the Cbl, Hakai, and SOCS-Cul5-RING ligase families, stimulate the ubiquitination of phosphotyrosine-containing proteins, including receptor and nonreceptor tyrosine kinases and their phosphorylated substrates. Because ubiquitination frequently routes proteins for degradation by the lysosome or proteasome, these E3 ligases are able to potently inhibit tyrosine kinase signaling. Their loss or mutational inactivation can contribute to cancer, autoimmunity, or endocrine disorders, such as diabetes. However, these ligases also have biological functions that are independent of their ubiquitination activity. Here we review relevant literature and then focus on more-recent developments in understanding the structures, substrates, and pathways through which the phosphotyrosine-specific ubiquitin ligases regulate diverse aspects of cell biology. Phosphorylation and ubiquitination are among the commonest and best-studied posttranslational modifications of proteins. A phosphate group or ubiquitin molecule can trigger or obstruct protein-protein interactions, alter subcellular localization, stabilize a particular protein conformation, or have myriad other effects. Phosphorylation is directly catalyzed by protein kinases, but ubiquitination is more complex, requiring sequential activity of E1, E2, and E3 ubiquitin-activating, -conjugating, and -ligating enzymes (1-5). E3 ubiquitin ligases fall into two major groups: HECT domain ligases receive ubiquitin from an E2 enzyme and transfer it to a bound substrate, while RING-type ligases position an E2-ubiquitin conjugate near a substrate protein to facilitate ubiquitin transfer. Both phosphorylation and ubiquitination are reversible; protein phosphorylation is reversed by protein phosphatases and ubiquitination by deubiquitinating enzymes (DUBs) (6-8). Therefore, both phosphorylation/dephosphorylation and ubiquitination/deubiquitination can allow repeated cycles of protein modification. Reversible ubiquitination is particularly important in DNA repair and NF-B signaling. However, many ubiquitination events lead irreversibly to protein destruction, allowing regulation of protein turnover. For example, K48 polyubiquitin chains primarily route cytosolic proteins to the proteasome, while modification of many Lys residues with single ubiquitin molecules (multimonoubiquitination) has several functions, including routing membrane proteins for destruction in the lysosome (9-11). The irreversibility of proteolysis means that the ubiquitin-proteasome and ubiquitin-lysosome pathways directly control protein life spans.Protein phosphorylation and ubiquitination cross talk at many levels (12). In this review, we focus on situations where phosphorylation of a substrate creates a binding site for an E3 ligase, rendering ubiquitination dependent on prior phosphorylation of that substrate (13). Such phosphorylation-dependent substrate selection has particular importance because it can layer negative feedback onto an otherwise reversible phosphoryla...

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The signaling suppressor CIS controls proallergic T cell development and allergic airway inflammation

Cited by 115 publications

References 69 publications

Systems analysis of sex differences reveals an immunosuppressive role for testosterone in the response to influenza vaccination

Systems analysis of sex differences reveals an immunosuppressive role for testosterone in the response to influenza vaccination

Prerequisites for Functional Interleukin 31 Signaling and Its Feedback Regulation by Suppressor of Cytokine Signaling 3 (SOCS3)

Cell Regulation by Phosphotyrosine-Targeted Ubiquitin Ligases

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