Varicellovirus UL49.5 proteins differentially affect the function of the transporter associated with antigen processing, TAP

• Published in: PLoS pathogens Vol. 4; no. 5; p. e1000080
• Main Authors: Koppers-Lalic, D, Verweij, M.C, Lipinska, A.D, Wang, Y, Quinten, E, Reits, E.A, Koch, J, Loch, S, Rezende, M.M, Daus, F.J, Bienkowska-Szewczyk, K, Osterrieder, N, Mettenleiter, T.C, Heemskerk, M.H.M, Tampe, R, Neefjes, J.J, Chowdhury, S.I, Ressing, M.E, Rijsewijk, F.A.M, Wiertz, E.J.H.J
• Format: Journal Article
• Language: English
• Published: San Francisco, USA Public Library of Science 01.05.2008
• Subjects: Bovine herpesvirus 1; Carrier proteins; cytomegalovirus us6 glycoprotein; Cytotoxicity; down-regulation; Equine herpesvirus; Equine herpesvirus 1; Experiments; finger protein; Genes; Herpesviruses; Immunology/Antigen Processing and Recognition; Immunology/Immunomodulation; ligase mk3; Lymphocytes; major histocompatibility complex; mhc class-i; molecular-mechanism; peptide-loading complex; Peptides; Physiological aspects; Proteins; Pseudorabies virus; Varicella-zoster virus; Varicellovirus; viral immune evasion; Viral infections; Viral proteins; Virology/Immune Evasion; Viruses
• ISSN: 1553-7366; 1553-7374; 1553-7374
• DOI: 10.1371/journal.ppat.1000080

Cytotoxic T-lymphocytes play an important role in the protection against viral infections, which they detect through the recognition of virus-derived peptides, presented in the context of MHC class I molecules at the surface of the infected cell. The transporter associated with antigen processing (TAP) plays an essential role in MHC class I--restricted antigen presentation, as TAP imports peptides into the ER, where peptide loading of MHC class I molecules takes place. In this study, the UL49.5 proteins of the varicelloviruses bovine herpesvirus 1 (BHV-1), pseudorabies virus (PRV), and equine herpesvirus 1 and 4 (EHV-1 and EHV-4) are characterized as members of a novel class of viral immune evasion proteins. These UL49.5 proteins interfere with MHC class I antigen presentation by blocking the supply of antigenic peptides through inhibition of TAP. BHV-1, PRV, and EHV-1 recombinant viruses lacking UL49.5 no longer interfere with peptide transport. Combined with the observation that the individually expressed UL49.5 proteins block TAP as well, these data indicate that UL49.5 is the viral factor that is both necessary and sufficient to abolish TAP function during productive infection by these viruses. The mechanisms through which the UL49.5 proteins of BHV-1, PRV, EHV-1, and EHV-4 block TAP exhibit surprising diversity. BHV-1 UL49.5 targets TAP for proteasomal degradation, whereas EHV-1 and EHV-4 UL49.5 interfere with the binding of ATP to TAP. In contrast, TAP stability and ATP recruitment are not affected by PRV UL49.5, although it has the capacity to arrest the peptide transporter in a translocation-incompetent state, a property shared with the BHV-1 and EHV-1 UL49.5. Taken together, these results classify the UL49.5 gene products of BHV-1, PRV, EHV-1, and EHV-4 as members of a novel family of viral immune evasion proteins, inhibiting TAP through a variety of mechanisms.