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Modelling of pathogen-host systems using deeper ORF annotations and transcriptomics to inform proteomics analyses

机译:使用更深的ORF注释和转录组织来告知蛋白质组学分析的病原体主机系统的建模

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The Zika virus is a flavivirus that can cause fulminant outbreaks and lead to Guillain-Barré syndrome, microcephaly and fetal demise. Like other flaviviruses, the Zika virus is transmitted by mosquitoes and provokes neurological disorders. Despite its risk to public health, no antiviral nor vaccine are currently available. In the recent years, several studies have set to identify human host proteins interacting with Zika viral proteins to better understand its pathogenicity. Yet these studies used standard human protein sequence databases. Such databases rely on genome annotations, which enforce a minimal open reading frame (ORF) length criterion. An ever-increasing number of studies have demonstrated the shortcomings of such annotation, which overlooks thousands of functional ORFs. Here we show that the use of a customized database including currently non-annotated proteins led to the identification of 4 alternative proteins as interactors of the viral capsid and NS4A proteins. Furthermore, 12 alternative proteins were identified in the proteome profiling of Zika infected monocytes, one of which was significantly up-regulated. This study presents a computational framework for the re-analysis of proteomics datasets to better investigate the viral-host protein interplays upon infection with the Zika virus.
机译:Zika病毒是一种可引起暴发性爆发并导致Guillain-Barré综合征,微微术和胎儿消亡的黄病毒。与其他黄病毒一样,Zika病毒由蚊子传播并引起神经系统疾病。尽管有风险对公共卫生,目前没有抗病毒和疫苗。在近年来,几项研究已经设定了与Zika病毒蛋白相互作用以更好地了解其致病性的人宿主蛋白。然而,这些研究使用标准人蛋白序列数据库。这些数据库依赖于基因组注释,这强制执行最小的开放阅读帧(ORF)长度标准。越来越多的研究已经证明了这种注释的缺点,这忽略了数千次功能性ORF。在这里,我们表明,使用包括当前未注释的蛋白质的定制数据库导致4替代蛋白质作为病毒衣壳和NS4A蛋白的交互蛋白。此外,在Zika感染的单核细胞的蛋白质组分析中鉴定了12种替代蛋白质,其中一个显着上调。该研究提出了一种计算框架,用于再分析蛋白质组学数据集,以更好地研究与Zika病毒感染的病毒宿主蛋白相互作用。

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