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鉴定出一种干扰素调节因子家族成员,其可与干扰素刺激反应元件结合并激活干扰素诱导基因的表达。

Identification of a member of the interferon regulatory factor family that binds to the interferon-stimulated response element and activates expression of interferon-induced genes.

作者信息

Au W C, Moore P A, Lowther W, Juang Y T, Pitha P M

机构信息

Oncology Center, Johns Hopkins University, Baltimore, MD 21231, USA.

出版信息

Proc Natl Acad Sci U S A. 1995 Dec 5;92(25):11657-61. doi: 10.1073/pnas.92.25.11657.

Abstract

A family of interferon (IFN) regulatory factors (IRFs) have been shown to play a role in transcription of IFN genes as well as IFN-stimulated genes. We report the identification of a member of the IRF family which we have named IRF-3. The IRF-3 gene is present in a single copy in human genomic DNA. It is expressed constitutively in a variety of tissues and no increase in the relative steady-state levels of IRF-3 mRNA was observed in virus-infected or IFN-treated cells. The IRF-3 gene encodes a 50-kDa protein that binds specifically to the IFN-stimulated response element (ISRE) but not to the IRF-1 binding site PRD-I. Overexpression of IRF-3 stimulates expression of the IFN-stimulated gene 15 (ISG15) promoter, an ISRE-containing promoter. The murine IFNA4 promoter, which can be induced by IRF-1 or viral infection, is not induced by IRF-3. Expression of IRF-3 as a Gal4 fusion protein does not activate expression of a chloramphenicol acetyltransferase reporter gene containing repeats of the Gal4 binding sites, indicating that this protein does not contain the transcription transactivation domain. The high amino acid homology between IRF-3 and ISG factor 3 gamma polypeptide (ISGF3 gamma) and their similar binding properties indicate that, like ISGF3 gamma, IRF-3 may activate transcription by complex formation with other transcriptional factors, possibly members of the Stat family. Identification of this ISRE-binding protein may help us to understand the specificity in the various Stat pathways.

摘要

干扰素(IFN)调节因子(IRF)家族已被证明在IFN基因以及IFN刺激基因的转录中发挥作用。我们报告了IRF家族一个成员的鉴定,我们将其命名为IRF-3。IRF-3基因在人类基因组DNA中以单拷贝形式存在。它在多种组织中组成性表达,在病毒感染或IFN处理的细胞中未观察到IRF-3 mRNA相对稳态水平的增加。IRF-3基因编码一种50 kDa的蛋白质,该蛋白质特异性结合IFN刺激反应元件(ISRE),但不结合IRF-1结合位点PRD-I。IRF-3的过表达刺激了IFN刺激基因15(ISG15)启动子的表达,该启动子含有ISRE。可被IRF-1或病毒感染诱导的小鼠IFNA4启动子,不能被IRF-3诱导。作为Gal4融合蛋白表达的IRF-3不激活含有Gal4结合位点重复序列的氯霉素乙酰转移酶报告基因的表达,表明该蛋白质不包含转录反式激活结构域。IRF-3与ISG因子3γ多肽(ISGF3γ)之间的高氨基酸同源性及其相似的结合特性表明,与ISGF3γ一样,IRF-3可能通过与其他转录因子(可能是Stat家族成员)形成复合物来激活转录。鉴定这种ISRE结合蛋白可能有助于我们理解各种Stat途径中的特异性。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/e406/40461/0106a9518c78/pnas01503-0347-a.jpg

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