β-（1→3）-D-葡聚糖调节核因子κB、AT和IL-6的DNA结合，导致IL-1β/IL-1受体拮抗剂比值发生抗炎性转变。

Beta-(1-->3)-D-glucan modulates DNA binding of nuclear factors kappaB, AT and IL-6 leading to an anti-inflammatory shift of the IL-1beta/IL-1 receptor antagonist ratio.

作者信息

Luhm Juergen, Langenkamp Ulrich, Hensel Jenny, Frohn Christoph, Brand Joerg M, Hennig Holger, Rink Lothar, Koritke Petra, Wittkopf Nadine, Williams David L, Mueller Antje

机构信息

Institute of Immunology and Transfusion Medicine, Medical School, University of Lübeck, Germany.

出版信息

BMC Immunol. 2006 Mar 22;7:5. doi: 10.1186/1471-2172-7-5.

DOI:10.1186/1471-2172-7-5

PMID:16553947

原文链接:https://pmc.ncbi.nlm.nih.gov/articles/PMC1472690/

Abstract

BACKGROUND

Beta-1-->3-D-glucans represent a pathogen-associated molecular pattern and are able to modify biological responses. Employing a comprehensive methodological approach, the aim of our in vitro study was to elucidate novel molecular and cellular mechanisms of human peripheral blood immune cells mediated by a fungal beta-1-->3-D-glucan, i.e. glucan phosphate, in the presence of lipopolysaccharide (LPS) or toxic shock syndrome toxin 1 (TSST-1).

RESULTS

Despite an activation of nuclear factor (NF) kappaB, NFinterleukin(IL)-6 and NFAT similar to LPS or TSST-1, we observed no significant production of IL-1beta, IL-6, tumor necrosis factor alpha or interferon gamma induced by glucan phosphate. Glucan phosphate-treated leukocytes induced a substantial amount of IL-8 (peak at 18 h: 5000 pg/ml), likely due to binding of NFkappaB to a consensus site in the IL-8 promoter. An increase in IL-1receptor antagonist (RA) production (peak at 24 h: 12000 pg/ml) by glucan phosphate-treated cells positively correlated with IL-8 levels. Glucan phosphate induced significant binding to a known NFIL-6 site and a new NFAT site within the IL-1RA promoter, which was confirmed by inhibition experiments. When applied in combination with either LPS or TSST-1 at the same time points, we detected that glucan phosphate elevated the LPS- and the TSST-1-induced DNA binding of NFkappaB, NFIL-6 and NFAT, leading to a synergistic increase of IL-1RA. Further, glucan phosphate modulated the TSST-1-induced inflammatory response via reduction of IL-1beta and IL-6. As a consequence, glucan phosphate shifted the TSST-1-induced IL-1beta/IL-1RA ratio towards an anti-inflammatory phenotype. Subsequently, glucan phosphate decreased the TSST-1-induced, IL-1-dependent production of IL-2.

CONCLUSION

Thus, beta-1-->3-D-glucans may induce beneficial effects in the presence of pro-inflammatory responses, downstream of receptor binding and signaling by switching a pro- to an anti-inflammatory IL-1RA-mediated reaction. Our results also offer new insights into the complex regulation of the IL-1RA gene, which can be modulated by a beta-1-->3-D-glucan.

摘要

背景

β-1,3-D-葡聚糖是一种病原体相关分子模式，能够改变生物学反应。采用全面的方法，我们体外研究的目的是阐明在脂多糖（LPS）或中毒性休克综合征毒素1（TSST-1）存在的情况下，真菌β-1,3-D-葡聚糖即磷酸葡聚糖介导的人外周血免疫细胞的新分子和细胞机制。

结果

尽管磷酸葡聚糖激活核因子（NF）κB、NF白细胞介素（IL）-6和NFAT的情况与LPS或TSST-1相似，但我们观察到磷酸葡聚糖未显著诱导IL-1β、IL-6、肿瘤坏死因子α或干扰素γ的产生。磷酸葡聚糖处理的白细胞诱导产生大量IL-8（18小时达到峰值：5000 pg/ml），这可能是由于NFκB与IL-8启动子中的共有序列结合。磷酸葡聚糖处理的细胞中IL-1受体拮抗剂（RA）产生增加（24小时达到峰值：12000 pg/ml），与IL-8水平呈正相关。磷酸葡聚糖诱导与IL-1RA启动子内已知的NFIL-6位点和新的NFAT位点显著结合，抑制实验证实了这一点。当在相同时间点与LPS或TSST-1联合应用时，我们检测到磷酸葡聚糖提高了LPS和TSST-1诱导的NFκB、NFIL-6和NFAT的DNA结合，导致IL-1RA协同增加。此外，磷酸葡聚糖通过降低IL-1β和IL-6来调节TSST-1诱导的炎症反应。结果，磷酸葡聚糖使TSST-1诱导的IL-1β/IL-1RA比值向抗炎表型转变。随后，磷酸葡聚糖降低了TSST-1诱导的、IL-1依赖性的IL-2产生。

结论

因此，β-1,3-D-葡聚糖在促炎反应存在的情况下，在受体结合和信号传导下游，通过将促炎反应转变为抗炎的IL-1RA介导的反应，可能诱导有益作用。我们的结果也为IL-1RA基因的复杂调控提供了新见解，该基因可被β-1,3-D-葡聚糖调节。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/0de5/1472690/e93fc3ebe1ca/1471-2172-7-5-1.jpg

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β-（1→3）-D-葡聚糖调节核因子κB、AT和IL-6的DNA结合，导致IL-1β/IL-1受体拮抗剂比值发生抗炎性转变。

Beta-(1-->3)-D-glucan modulates DNA binding of nuclear factors kappaB, AT and IL-6 leading to an anti-inflammatory shift of the IL-1beta/IL-1 receptor antagonist ratio.

作者信息

Luhm Juergen, Langenkamp Ulrich, Hensel Jenny, Frohn Christoph, Brand Joerg M, Hennig Holger, Rink Lothar, Koritke Petra, Wittkopf Nadine, Williams David L, Mueller Antje

机构信息

Institute of Immunology and Transfusion Medicine, Medical School, University of Lübeck, Germany.