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严重急性呼吸综合征冠状病毒nsp3的PLnc结构域作为一种复制/转录支架蛋白。

The SARS-Coronavirus PLnc domain of nsp3 as a replication/transcription scaffolding protein.

作者信息

Imbert Isabelle, Snijder Eric J, Dimitrova Maria, Guillemot Jean-Claude, Lécine Patrick, Canard Bruno

机构信息

Centre National de la Recherche Scientifique and Universités d'Aix-Marseille I et II, UMR 6098, Architecture et Fonction des Macromolécules Biologiques, Ecole Supérieure d'Ingénieurs de Luminy-Case 925, Marseille Cedex 9, France.

出版信息

Virus Res. 2008 May;133(2):136-48. doi: 10.1016/j.virusres.2007.11.017. Epub 2008 Feb 5.

Abstract

Many genetic and mechanistic features distinguish the coronavirus replication machinery from that encoded by most other RNA viruses. The coronavirus replication/transcription complex is an assembly of viral and, most probably, cellular proteins that mediate the synthesis of both the unusually large (approximately 30 kb) RNA genome and an extensive set of subgenomic mRNAs. The viral components of the complex are encoded by the giant replicase gene, which is expressed in the form of two polyproteins (pp1a and pp1ab) that are processed into 16 cleavage products (nonstructural proteins 1-16). Using the combination of yeast two-hybrid screening and GST pull-down assays, we have now analyzed all potential interactions between SARS-Coronavirus nonstructural proteins, which may contribute to the structure and/or function of the viral replication/transcription complex. We demonstrate the existence of a complex network of interactions involving all 16 nonstructural proteins. Our results both confirmed previously described associations and identified novel heterodimerizations. The interaction map thus provides a sum of the interactions that may occur at some point during coronavirus RNA synthesis and provides a framework for future research.

摘要

许多遗传和机制特征使冠状病毒的复制机制有别于大多数其他RNA病毒所编码的机制。冠状病毒复制/转录复合体是病毒蛋白以及极有可能的细胞蛋白的集合体,介导了异常大的(约30 kb)RNA基因组和一系列亚基因组mRNA的合成。该复合体的病毒成分由巨大的复制酶基因编码,该基因以两种多聚蛋白(pp1a和pp1ab)的形式表达,这两种多聚蛋白会被加工成16种裂解产物(非结构蛋白1-16)。利用酵母双杂交筛选和GST下拉试验相结合的方法,我们现在分析了严重急性呼吸综合征冠状病毒非结构蛋白之间所有可能的相互作用,这些相互作用可能有助于病毒复制/转录复合体的结构和/或功能。我们证明了存在一个涉及所有16种非结构蛋白的复杂相互作用网络。我们的结果既证实了先前描述的关联,又鉴定出了新的异源二聚体。因此,相互作用图谱总结了冠状病毒RNA合成过程中某个时刻可能发生的相互作用,并为未来的研究提供了一个框架。

https://cdn.ncbi.nlm.nih.gov/pmc/blobs/ed85/7114086/3e38e4d5a622/gr1.jpg

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