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首页> 外文期刊>PLoS One >iTRAQ-based high-throughput proteomics analysis reveals alterations of plasma proteins in patients infected with human bocavirus
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iTRAQ-based high-throughput proteomics analysis reveals alterations of plasma proteins in patients infected with human bocavirus

机译:基于ITRAQ的高通量蛋白质组学分析揭示了用人类Bocavirus感染的患者血浆蛋白的改变

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Human bocavirus (HBoV) is a member of the genus Bocavirus , family Parvoviridae , and subfamily Parvovirus and was first identified in nasopharyngeal aspirates of Swedish children with acute respiratory tract infection (ARTI) in 2005. It is the causative agent of nasopharyngeal aspirate disease and death in children. The HboV genomic structure is a linear single-stranded DNA (ssDNA). Its clinical pathogenic characteristics have been extensively studied, however, at present the molecular mechanism underlying the pathogenesis of HBoV infection is not completely clear. In this study, a total of 293 differentially expressed proteins (DEPs) between ARTI cases and healthy plasma samples were characterized using isobaric tags for relative and absolute quantitation (iTRAQ)-coupled bioinformatics analysis, among which 148 were up-regulated and 135 were down-regulated. Gene Ontology (GO) and Cluster of Orthologous Groups of proteins (COG) annotated an enrichment of DEPs in complement activation and biological processes like immunity, inflammation, signal transduction, substance synthesis, and metabolism. Kyoto Encyclopedia of Genes and Genomes (KEGG) analysis enriched DEPs mainly in the Wnt signaling pathway (ko04310), PPAR signaling pathway (ko03320), intestinal immune network for IgA production (ko04672), complement and coagulation cascades (ko04610), Toll-like receptor signaling pathway (ko04620) and B cell receptor signaling pathway (ko04662). Further, expression levels of three candidate proteins (upregulated PPP2R1A and CUL1, and downregulated CETP) were validated using western blotting. Our investigation is the first analysis of the proteomic profile of HBoV-infected ARTI cases using the iTRAQ approach, providing a foundation for a better molecular understanding of the pathogenesis of ARTI in children.
机译:人类博克苏斯(HBOV)是Bocavirus,Family Parvoviridae和亚家族剖视病毒的成员,并于2005年首次在瑞典呼吸道感染(ARTI)的鼻咽血液儿童中鉴定为鼻咽血液儿童。它是鼻咽吸汗疾病的致病因子孩子死亡。 HBoV基因组结构是直链单链DNA(SSDNA)。其临床致病特性已被广泛研究,然而,目前HBOV感染的发病机制的分子机制并不完全清楚。在该研究中,使用ARTI病例和健康等离子体样品之间的总共293个差异表达蛋白质(DEP),用于使用同位数和绝对定量(ITRAQ) - 耦合的生物信息学分析,其中148次上调,135次下降 - 解释。基因本体(GO)和局部蛋白质组(COG)群(COG)注释了富含免疫,炎症,信号转导,物质合成和代谢等补体激活和生物方法的富集的富集。基因和基因组(Kegg)的京都百科全书(Kegg)分析主要在WNT信号通路(KO04310),PPAR信号通路(KO03320),用于IgA生产的肠道免疫网络(KO04672),补体和凝血级联(KO04610),收费受体信号通路(KO04620)和B细胞受体信号传导途径(KO04662)。此外,使用蛋白质印迹验证了三种候选蛋白的表达水平(上调PPP2R1A和CUL1和下调的CET)。我们的调查是利用ITRAQ方法对HBOV感染的ARTI病例的蛋白质表征的第一次分析,为儿童ARTI发病机制提供了更好的分子理解基础。

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