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首页> 外文期刊>Journal of interferon and cytokine research: The official journal of the International Society for Interferon and Cytokine Research >Interferon-stimulated response element (ISRE)-binding protein complex DRAF1 is activated in Sindbis virus (HR)-infected cells.
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Interferon-stimulated response element (ISRE)-binding protein complex DRAF1 is activated in Sindbis virus (HR)-infected cells.

机译:干扰素刺激的反应元件(ISRE)结合蛋白复合物DRAF1在Sindbis病毒(HR)感染的细胞中被激活。

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摘要

To elucidate the host cell defense mechanisms in response to Sindbis viral infection, we have started to characterize interferon (IFN)-stimulated response element (ISRE)-binding proteins activated in infected cells that are involved in the transcriptional induction of IFN type I-inducible genes. Using electromobility shift assays (EMSA), we detected several protein complexes with a human IFN-stimulated gene 15 (ISG15) ISRE in extracts from virus-infected L929 cells that were absent in extracts from uninfected cells. Comigration with Newcastle disease virus-activated ISRE-binding complexes, ISRE-binding specificity, supershift experiments, and conditions of formation indicate that the complexes activated by Sindbis viral infection in L929 cells correspond to DRAF1 and ISG factor 3 (ISGF3). Transfection of L929 cells with poly rI:rC induced only ISGF3. DRAF1 could be detected in Sindbis virus-infected mouse embryo fibroblasts derived from IFNR type I and type II KO mice. Viral RNA synthesis is required for activation of DRAF1.
机译:为了阐明响应辛德比斯病毒感染的宿主细胞防御机制,我们已开始鉴定在感染细胞中激活的干扰素(IFN)刺激的反应元件(ISRE)结合蛋白,这些蛋白参与了IFN-I诱导型的转录诱导基因。使用电动迁移率分析(EMSA),我们在病毒感染的L929细胞的提取物中检测到几种与人IFN刺激基因15(ISG15)ISRE形成的蛋白质复合物,而在未感染的细胞提取物中则没有。与新城疫病毒激活的ISRE结合复合物,ISRE结合特异性,超移位实验和形成条件的研究表明,L929细胞中Sindbis病毒感染激活的复合物对应于DRAF1和ISG因子3(ISGF3)。用poly rI:rC转染L929细胞仅诱导ISGF3。 DRAF1可以在源于IFNR I型和II型KO小鼠的Sindbis病毒感染的小鼠胚胎成纤维细胞中检测到。病毒RNA合成是激活DRAF1所必需的。

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