Ablation of the Regulatory IE1 Protein of Murine Cytomegalovirus Alters In Vivo Pro-inflammatory TNF-alpha Production during Acute Infection

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RESEARCH PRODUCT

Ablation of the Regulatory IE1 Protein of Murine Cytomegalovirus Alters In Vivo Pro-inflammatory TNF-alpha Production during Acute Infection

William J. Britt Sara Rodríguez-martín Kai Alexander Kropp Vanessa Wilhelmi Vanda Juranic Lisnic Wei Yuan Hsieh Mathieu Blanc Andrew Livingston Andreas Busche Hille Tekotte Martin Messerle Manfred Auer Iain Fraser Stipan Jonjić Ana Angulo Matthias J. Reddehase Peter Ghazal

subject

Male Cytomegalovirus Infection Muromegalovirus Viral Diseases medicine.medical_treatment viruses TNF TNF-alpha murine cytomegalovirus MCMV IE Virus Replication Mice 0302 clinical medicine Gene expression Biology (General)Mice Inbred BALB C 0303 health sciences education.field_of_study Physics virus diseases Herpesviridae Infections Transfection 3. Good health Genètica microbiana Interleukin 10 Phenotype Infectious Diseases Cytokine Liver Cytokines Medicine Female Tumor necrosis factor alpha BIOMEDICINA I ZDRAVSTVO. Temeljne medicinske znanosti.Microbial genetics Signal Transduction Research Article DNA Replication Gene Expression Regulation Viral QH301-705.5 Immunology Population Biology Microbiology Cell Line Immediate-Early Proteins Viral Proteins 03 medical and health sciences In vivo Virology Genetics medicine Animals education Molecular Biology 030304 developmental biology Tumor Necrosis Factor-alpha Macrophages BIOMEDICINE AND HEALTHCARE. Basic Medical Sciences.Física RC581-607 Mice Inbred C57BL Viral replication DNA Viral Immunology Parasitology Immunologic diseases. Allergy 030215 immunology

description

Little is known about the role of viral genes in modulating host cytokine responses. Here we report a new functional role of the viral encoded IE1 protein of the murine cytomegalovirus in sculpting the inflammatory response in an acute infection. In time course experiments of infected primary macrophages (MΦs) measuring cytokine production levels, genetic ablation of the immediate-early 1 (ie1) gene results in a significant increase in TNFα production. Intracellular staining for cytokine production and viral early gene expression shows that TNFα production is highly associated with the productively infected MΦ population of cells. The ie1- dependent phenotype of enhanced MΦ TNFα production occurs at both protein and RNA levels. Noticeably, we show in a series of in vivo infection experiments that in multiple organs the presence of ie1 potently inhibits the pro-inflammatory cytokine response. From these experiments, levels of TNFα, and to a lesser extent IFNβ, but not the anti-inflammatory cytokine IL10, are moderated in the presence of ie1. The ie1- mediated inhibition of TNFα production has a similar quantitative phenotype profile in infection of susceptible (BALB/c) and resistant (C57BL/6) mouse strains as well as in a severe immuno-ablative model of infection. In vitro experiments with infected macrophages reveal that deletion of ie1 results in increased sensitivity of viral replication to TNFα inhibition. However, in vivo infection studies show that genetic ablation of TNFα or TNFRp55 receptor is not sufficient to rescue the restricted replication phenotype of the ie1 mutant virus. These results provide, for the first time, evidence for a role of IE1 as a regulator of the pro-inflammatory response and demonstrate a specific pathogen gene capable of moderating the host production of TNFα in vivo.

year	journal	country	edition	language
2012-08-30

10.1371/journal.ppat.1002901 https://www.pure.ed.ac.uk/ws/files/7933754/Ablation_of_the_Regulatory_IE1_Protein_of_Murine_Cytomegalovirus_Alters_In_Vivo_Pro_inflammatory_TNF_alpha_Production_during_Acute_Infection.pdf