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Quantitative phosphoproteome on the silkworm (Bombyx mori) cells infected with baculovirus

机译:蚕茧(Bombyx Mori)细胞的定量磷酸溶细胞感染杆状病毒

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Abstract Background Bombyx mori has become an important model organism for many fundamental studies. Bombyx mori nucleopolyhedrovirus (BmNPV) is a significant pathogen to Bombyx mori, yet also an efficient vector for recombinant protein production. A previous study indicated that acetylation plays many vital roles in several cellular processes of Bombyx mori while global phosphorylation pattern upon BmNPV infection remains elusive. Method Employing tandem mass tag (TMT) labeling and phosphorylation affinity enrichment followed by high-resolution LC-MS/MS analysis and intensive bioinformatics analysis, the quantitative phosphoproteome in Bombyx mori cells infected by BmNPV at 24 hpi with an MOI of 10 was extensively examined. Results Totally, 6480 phosphorylation sites in 2112 protein groups were identified, among which 4764 sites in 1717 proteins were quantified. Among the quantified proteins, 81 up-regulated and 25 down-regulated sites were identified with significant criteria (the quantitative ratio above 1.3 was considered as up-regulation and below 0.77 was considered as down-regulation) and with significant p-value (p < 0.05). Some proteins of BmNPV were also hyperphosphorylated during infection, such as P6.9, 39 K, LEF-6, Ac58-like protein, Ac82-like protein and BRO-D. Conclusion The phosphorylated proteins were primary involved in several specific functions, out of which, we focused on the binding activity, protein synthesis, viral replication and apoptosis through kinase activity.
机译:摘要背景Bombyx Mori已成为许多基本研究的重要模型生物。 Bombyx Mori核多肽(BMNPV)是Bombyx Mori的重要病原体,但也是重组蛋白质产生的有效载体。先前的研究表明,乙酰化在Bombyx Mori的几种细胞过程中起着许多重要作用,而BMNPV感染的全局磷酸化模式仍然难以捉摸。方法用人串联质量标签(TMT)标签和磷酸化亲和富集,随后高分辨率LC-MS / MS分析和密集的生物信息学分析,在家蚕细胞中的定量磷酸化蛋白质在24 HPI由多角体病毒感染的10的MOI进行了广泛研究。结果完全,鉴定了2112个蛋白质基团中的6480个磷酸化位点,其中量化了1717个蛋白质中的4764位点。在定量的蛋白质中,以显着标准鉴定出现的蛋白质,81个上调和25个下调位点(将1.3高于1.3的定量比例,被认为是上调,低于0.77被认为是下调的),并且具有显着的p值(p <0.05)。在感染期间,BMNPV的一些蛋白质也是高磷酸化,例如P6.9,39 K,LEF-6,AC58样蛋白,AC82样蛋白和BRO-D。结论磷酸化蛋白初级涉及几种特定功能,其中,我们专注于通过激酶活性的结合活性,蛋白质合成,病毒复制和细胞凋亡。

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