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首页> 美国卫生研究院文献>The Journal of Experimental Medicine >Interferon (IFN) beta acts downstream of IFN-gamma-induced class II transactivator messenger RNA accumulation to block major histocompatibility complex class II gene expression and requires the 48- kD DNA-binding protein ISGF3-gamma
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Interferon (IFN) beta acts downstream of IFN-gamma-induced class II transactivator messenger RNA accumulation to block major histocompatibility complex class II gene expression and requires the 48- kD DNA-binding protein ISGF3-gamma

机译:干扰素(IFN)β在IFN-γ诱导的II类反式激活子信使RNA积累的下游起作用以阻止主要的组织相容性复合物II类基因的表达并需要48 kD DNA结合蛋白ISGF3-γ

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摘要

Interferon (IFN) gamma, a cardinal proinflammatory cytokine, induces expression of the gene products of the class II locus of the major histocompatibility complex (MHC), whereas IFN-alpha or -beta suppresses MHC class II expression. The mechanism of IFN-beta-mediated MHC class II inhibition has been unclear. Recently, a novel factor termed class II transactivator (CIITA) has been identified as essential for IFN- gamma-induced MHC class II transcription. We studied the status of IFN- gamma-induced CIITA messenger RNA (mRNA) accumulation and CIITA-driven transactivation in IFN-beta-treated cells and used cell lines that had defined defects in the type I IFN response pathway to address the roles of IFN signaling components in the inhibition of MHC class II induction. IFN-beta treatment did not suppress IFN-gamma-induced accumulation of CIITA mRNA. After cells were stably transfected with CIITA, endogenous MHC class II genes were constitutively expressed, and MHC class II promoters, delivered by transfection, were actively transcribed in CIITA-expressing cells. Expression of these promoters was significantly impaired by pretreatment with IFN-beta. These results suggest that IFN-beta acts downstream of CIITA mRNA accumulation, and acts in part by reducing the functional competence of CIITA for transactivating MHC class II promoters. IFN stimulated gene factor 3 (ISGF3) gamma was essential for IFN-beta to mediate inhibition of MHC class II induction, regardless of whether MHC class II transcription was stimulated by IFN-gamma or directly by CIITA expression. Results of these experiments suggest that inhibition of MHC class II in IFN-beta- treated cells requires expression of gene(s) directed by the ISGF3-IFN- stimulated response element pathway, and that these gene product(s) may act by blocking CIITA-driven transcription of MHC class II promoters.
机译:干扰素(IFN)γ是主要的促炎细胞因子,可诱导主要组织相容性复合物(MHC)的II类基因座的基因产物表达,而IFN-α或-β则抑制MHC II类表达。尚不清楚IFN-β介导的II类MHC抑制的机制。最近,一种被称为II类反式激活因子(CIITA)的新型因子已被确定为IFN-γ诱导的MHC II类转录所必需的。我们研究了在IFN-beta处理的细胞中IFN-γ诱导的CIITA信使RNA(mRNA)积累和CIITA驱动的反式激活的状态,并使用已在I型IFN反应途径中定义缺陷的细胞系来解决IFN的作用抑制MHC II类诱导的信号传导成分。 IFN-β处理不能抑制IFN-γ诱导的CIITA mRNA积累。用CIITA稳定转染细胞后,内源性MHC II类基因组成性表达,并通过转染递送的MHC II类启动子在表达CIITA的细胞中主动转录。用IFN-β预处理显着损害了这些启动子的表达。这些结果表明,IFN-β在CIITA mRNA积累的下游起作用,并且部分地通过降低CIITA反式激活MHC II类启动子的功能来起作用。 IFN刺激的基因因子3(ISGF3)γ对于IFN-β介导抑制MHC II类诱导至关重要,无论MHC II类转录是被IFN-γ刺激还是直接由CIITA表达刺激。这些实验的结果表明,在经IFN-β处理的细胞中抑制II类MHC的表达需要表达由ISGF3-IFN刺激的应答元件途径指导的基因,并且这些基因产物可能通过阻断CIITA发挥作用驱动的MHC II类启动子转录。

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