Plasmacytoid DCs (pDCs) are crucial mediators in the establishment of immunity against most viruses, given their extraordinary capacity to produce a massive quantity of type I IFN. In this study we investigate the response of pDCs to infection with EBV, a γ-herpes virus that persists with an asymptomatic infection in immunocompetent hosts, although in certain conditions it can promote development of cancers or autoimmune diseases. We show that high amounts of type I IFNs were released from isolated pDCs after exposure to EBV by a mechanism requiring TLRs and a functional autophagic machinery. We next demonstrate that EBV can infect pDCs via viral binding to MHC class II molecule HLA-DR and that pDCs express EBV-induced latency genes. Furthermore, we observe that EBV is able to induce activation but not maturation of pDCs, which correlates with an impaired TNF-α release. Accordingly, EBV-infected pDCs are unable to mount a full T-cell response, suggesting that impaired pDC maturation, combined with a concomitant EBV-mediated upregulation of the T-cell inhibitory molecules B7-H1 and ICOS-L, could represent an immune-evasion strategy promoted by the virus. These mechanisms might lead to persistence in immunocompetent hosts or to dysregulated immune responses linked to EBV-associated diseases.Keywords: EBV r Plasmacytoid DC r TLR r Type I IFN Additional supporting information may be found in the online version of this article at the publisher's web-site Introduction EBV, a γ-herpes virus with the ability to infect the majority of human population, persists in a latent asymptomatic infection Correspondence: Dr. Eliana Marina Coccia e-mail: eliana.coccia@iss.it for the lifetime of the host. In rare cases, EBV transforming capacity might promote development of different lymphomas or nasopharyngeal and gastric carcinomas [1]. Dysregulated immune responses to EBV have also been associated with development and/or pathogenesis of several autoimmune diseases, such as rheumatoid arthritis, systemic lupus erythematosus, and multiple sclerosis [2].C 2012 WILEY-VCH Verlag GmbH & Co. KGaA, Weinheim www.eji-journal.eu
148Martina Severa et al. Eur. J. Immunol. 2013. 43: 147-158 After infection of naïve B cells, EBV normally establishes different programs of latency, where up to nine EBV-encoded proteins can be expressed: six EBV nuclear antigens (EBNAs) and three latent membrane proteins (LMP1, LMP2A, LMP2B). Two types of EBV-encoded nontranslated RNAs are also transcribed in latently infected B cells: EBERs (small nonpolyadenylated, noncoding dsRNAs, expressed in all known forms of viral latency) and BARTs (BAMH1-A rightward transcripts). Memory B cells are the long-term EBV reservoir and express either no viral genes or only LMP2A (latency 0) [1,3].EBV has elaborated many strategies to evade immune surveillance, a feature of key importance to establish a successful life-long infection. Therefore, it is not surprising that several proteins that are encoded by the EBV genome are devoted to counteract the host immune response a...
