Guerra Susana, Nájera José Luis, González José Manuel, López-Fernández Luis A, Climent Nuria, Gatell José M, Gallart Teresa, Esteban Mariano
Department of Molecular and Cellular Biology, Centro Nacional de Biotecnología, Consejo Superior de Investigaciones Científicas, Campus Universidad Autónoma, E-28049 Madrid, Spain.
J Virol. 2007 Aug;81(16):8707-21. doi: 10.1128/JVI.00444-07. Epub 2007 May 30.
Although recombinants based on the attenuated poxvirus vectors MVA and NYVAC are currently in clinical trials, the nature of the genes triggered by these vectors in antigen-presenting cells is poorly characterized. Using microarray technology and various analysis conditions, we compared specific changes in gene expression profiling following MVA and NYVAC infection of immature human monocyte-derived dendritic cells (MDDC). Microarray analysis was performed at 6 h postinfection, since these viruses induced extensive cytopathic effects, rRNA breakdown, and apoptosis at late times postinfection. MVA- and NYVAC-infected MDDC shared upregulation of 195 genes compared to uninfected cells: MVA specifically upregulated 359 genes, and NYVAC upregulated 165 genes. Microarray comparison of NYVAC and MVA infection revealed 544 genes with distinct expression patterns after poxvirus infection and 283 genes specifically upregulated after MVA infection. Both vectors upregulated genes for cytokines, cytokine receptors, chemokines, chemokine receptors, and molecules involved in antigen uptake and processing, including major histocompatibility complex genes. mRNA levels for interleukin 12beta (IL-12beta), beta interferon, and tumor necrosis factor alpha were higher after MVA infection than after NYVAC infection. The expression profiles of transcription factors such as NF-kappaB/Rel and STAT were regulated similarly by both viruses; in contrast, OASL, MDA5, and IRIG-I expression increased only during MVA infection. Type I interferon, IL-6, and Toll-like receptor pathways were specifically induced after MVA infection. Following MVA or NYVAC infection in MDDC, we found similarities as well as differences between these virus strains in the expression of cellular genes with immunological function, which should have an impact when these vectors are used as recombinant vaccines.
尽管基于减毒痘病毒载体MVA和NYVAC的重组体目前正处于临床试验阶段,但这些载体在抗原呈递细胞中触发的基因的性质却鲜为人知。我们使用微阵列技术和各种分析条件,比较了未成熟的人单核细胞衍生树突状细胞(MDDC)在感染MVA和NYVAC后基因表达谱的特定变化。由于这些病毒在感染后期会诱导广泛的细胞病变效应、rRNA降解和细胞凋亡,因此在感染后6小时进行微阵列分析。与未感染细胞相比,感染MVA和NYVAC的MDDC共有195个基因上调:MVA特异性上调359个基因,NYVAC上调165个基因。NYVAC和MVA感染的微阵列比较显示,痘病毒感染后有544个基因具有不同的表达模式,MVA感染后有283个基因特异性上调。两种载体均上调了细胞因子、细胞因子受体、趋化因子、趋化因子受体以及参与抗原摄取和加工的分子的基因,包括主要组织相容性复合体基因。MVA感染后白细胞介素12β(IL-12β),β干扰素和肿瘤坏死因子α的mRNA水平高于NYVAC感染后。两种病毒对NF-κB/Rel和STAT等转录因子的表达谱调节相似;相反,OASL、MDA5和IRIG-I的表达仅在MVA感染期间增加。MVA感染后特异性诱导I型干扰素、IL-6和Toll样受体途径。在MDDC中感染MVA或NYVAC后,我们发现这些病毒株在具有免疫功能的细胞基因表达方面既有相似之处也有不同之处,这在将这些载体用作重组疫苗时应该会产生影响。
