首页> 外文期刊>Journal of drug targeting >Toward functional analysis of protein interactome using 'in vitro virus': in silico analyses of Fos/Jun interactors.
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Toward functional analysis of protein interactome using 'in vitro virus': in silico analyses of Fos/Jun interactors.

机译:使用“体外病毒”进行蛋白质相互作用组的功能分析:Fos / Jun相互作用因子的计算机分析。

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Our high-throughput in vitro virus (IVV) method for selection of protein-protein interactions (PPI) and complexes, based on a simple cell-free co-translation and selection followed by computational sequence data analysis, was previously used to identify 31 Fos and Jun interactors. Here, in silico analyses of biological function, localization and phenotype of these AP-1 (Fos/Jun) interactors were performed. The results suggest that Fos and Jun do not necessarily work together, but also interact separately with novel interactors, including products of disease-related genes. Fos showed transcription-related activities, while Jun interacted with motor-related and structural proteins. The reliability of the IVV selection for the Fos interactors was further confirmed by means of in vitro reciprocal prey and bait protein experiments and co-immunoprecipitation. Further study of these novel interactors may provide clues to new pathways or mechanisms of biological functions and diseases.
机译:我们基于简单的无细胞共翻译和选择,然后进行计算序列数据分析的高通量体外病毒(IVV)方法,用于选择蛋白质-蛋白质相互作用(PPI)和复合物,以前用于鉴定31种Fos和Jun的互动者。在这里,对这些AP-1(Fos / Jun)相互作用子的生物学功能,定位和表型进行了计算机分析。结果表明,Fos和Jun不一定协同工作,但也可以与新的相互作用因子(包括疾病相关基因的产物)单独相互作用。 Fos显示出转录相关活性,而Jun则与运动相关和结构蛋白相互作用。通过体外交互的猎物和诱饵蛋白实验以及免疫共沉淀进一步证实了针对Fos相互作用子的IVV选择的可靠性。对这些新型相互作用物的进一步研究可能为生物学功能和疾病的新途径或机制提供线索。

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