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人干扰素λ-1(IFN-λ1/IL-29)调节Th1/Th2反应。

Human interferon lambda-1 (IFN-lambda1/IL-29) modulates the Th1/Th2 response.

作者信息

Jordan W J, Eskdale J, Srinivas S, Pekarek V, Kelner D, Rodia M, Gallagher G

机构信息

Department of Oral Biology, New Jersey Dental School, Newark, NJ, USA.

出版信息

Genes Immun. 2007 Apr;8(3):254-61. doi: 10.1038/sj.gene.6364382. Epub 2007 Mar 15.

Abstract

Interferon lambda-1 (IFN-lambda1/IL-29) is a member of the Type-III interferon family, which contains three ligands: IFN-lambda1, 2 and 3. These three ligands use the same unique heterodimeric receptor composed of CRF2-12 (IFN-lambda-R1/IL-28Ralpha) and CRF2-4 (IL10-R-beta) chains. Like their close relatives, the Type-I interferons, IFN-lambda1, 2 and 3, promote the phosphorylation of STAT1 and STAT2, induce the ISRE3 complex, elevate OAS and MxA expression and exhibit antiviral activity in vitro. Their use of the IL10-R-beta chain and their ability to phosphorylate STAT3, STAT4 and STAT5 suggested that they may also exhibit immunomodulatory activity; their antiviral action led us to hypothesize that this activity might be directed toward the Th1/Th2 system. Here, we have demonstrated that IFN-lambda1 altered the activity of Th cells in three separate experimental systems: (i) mitogen stimulation, (ii) mixed-lymphocyte reaction (MLR) and (iii) stimulation of naive T cells by monocyte-derived dendritic cells (mDC). In Con-A stimulation assays, the inclusion of IFN-lambda1 consistently led to markedly diminished levels of secreted interleukin (IL-13) with occasional coincident, modest elevation of secreted IFN-gamma. IL-13 secretion was 100-fold more sensitive to IFN-lambda1 than was IFN-gamma secretion. These observations were also made in the allogeneic two-way MLR. IFN-lambda1 was able to alter cytokine-mediated Th biasing and when naive T cells were exposed to allogeneic mDC that had been matured in the presence of IFN-lambda1, secreted IL-13 was again markedly and consistently reduced, whereas secreted IFN-gamma was largely unaltered. These functions were independent of IL-10. Our data support a hitherto unsuspected role for IFN-lambda1 in modulating the development of Th1 and Th2 cells, with an apparent emphasis on the diminution of IL-13 secretion.

摘要

干扰素λ-1(IFN-λ1/IL-29)是III型干扰素家族的成员,该家族包含三种配体:IFN-λ1、2和3。这三种配体使用由CRF2-12(IFN-λ-R1/IL-28Rα)和CRF2-4(IL10-R-β)链组成的相同独特异二聚体受体。与它们的近亲I型干扰素一样,IFN-λ1、2和3促进STAT1和STAT2的磷酸化,诱导ISRE3复合物,提高OAS和Mx A的表达,并在体外表现出抗病毒活性。它们对IL10-R-β链的利用以及磷酸化STAT3、STAT4和STAT5的能力表明它们也可能具有免疫调节活性;它们的抗病毒作用使我们推测这种活性可能针对Th1/Th2系统。在这里,我们已经证明IFN-λ1在三个独立的实验系统中改变了Th细胞的活性:(i)丝裂原刺激,(ii)混合淋巴细胞反应(MLR)和(iii)单核细胞衍生的树突状细胞(mDC)对初始T细胞的刺激。在Con-A刺激试验中,加入IFN-λ1始终导致分泌的白细胞介素(IL-13)水平显著降低,偶尔同时出现分泌的IFN-γ适度升高。IL-13分泌对IFN-λ1的敏感性比IFN-γ分泌高100倍。在同种异体双向MLR中也观察到了这些现象。IFN-λ1能够改变细胞因子介导的Th偏向,当初始T细胞暴露于在IFN-λ1存在下成熟的同种异体mDC时,分泌的IL-13再次显著且持续减少,而分泌的IFN-γ基本未改变。这些功能独立于IL-10。我们的数据支持IFN-λ1在调节Th1和Th2细胞发育中迄今未被怀疑的作用,明显侧重于减少IL-13的分泌。

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