Vaccinia Virus Uses Retromer-Independent Cellular Retrograde Transport Pathways To Facilitate the Wrapping of Intracellular Mature Virions during Virus Morphogenesis

Kate Harrison; Ismar R Haga; Tali Pechenick Jowers; Seema Jasim; Jean-Christophe Cintrat; Daniel Gillet; Thomas Schmitt-John; Paul Digard; Philippa M Beard

doi:10.1128/JVI.01464-16

Vaccinia Virus Uses Retromer-Independent Cellular Retrograde Transport Pathways To Facilitate the Wrapping of Intracellular Mature Virions during Virus Morphogenesis

J Virol. 2016 Oct 28;90(22):10120-10132. doi: 10.1128/JVI.01464-16. Print 2016 Nov 15.

Authors

Affiliations

¹ The Roslin Institute and Royal (Dick) School of Veterinary Studies, University of Edinburgh, Roslin, Midlothian, United Kingdom.
² The Pirbright Institute, Pirbright, Surrey, United Kingdom.
³ SCBM, Institute of Biology and Technology of Saclay, CEA, LabEx LERMIT, Université Paris-Saclay, Gif Sur Yvette, France.
⁴ SIMOPRO, Institute of Biology and Technology of Saclay, CEA, LabEx LERMIT, Université Paris-Saclay, Gif Sur Yvette, France.
⁵ Molecular Biology and Genetics, Aarhus University, Aarhus, Denmark.
⁶ The Pirbright Institute, Pirbright, Surrey, United Kingdom pip.beard@roslin.ed.ac.uk.

Abstract

Poxviruses, such as vaccinia virus (VACV), undertake a complex cytoplasmic replication cycle which involves morphogenesis through four distinct virion forms and includes a crucial wrapping step whereby intracellular mature virions (IMVs) are wrapped in two additional membranes to form intracellular enveloped virions (IEVs). To determine if cellular retrograde transport pathways are required for this wrapping step, we examined VACV morphogenesis in cells with reduced expression of the tetrameric tethering factor known as the GARP (Golgi-associated retrograde pathway), a central component of retrograde transport. VACV multistep replication was significantly impaired in cells transfected with small interfering RNA targeting the GARP complex and in cells with a mutated GARP complex. Detailed analysis revealed that depletion of the GARP complex resulted in a reduction in the number of IEVs, thereby linking retrograde transport with the wrapping of IMVs. In addition, foci of viral wrapping membrane proteins without an associated internal core accumulated in cells with a mutated GARP complex, suggesting that impaired retrograde transport uncouples nascent IMVs from the IEV membranes at the site of wrapping. Finally, small-molecule inhibitors of retrograde transport strongly suppressed VACV multistep growth in vitro and reduced weight loss and clinical signs in an in vivo murine model of systemic poxviral disease. This work links cellular retrograde transport pathways with the morphogenesis of poxviruses and identifies a panel of novel inhibitors of poxvirus replication. IMPORTANCE Cellular retrograde transport pathways traffic cargo from endosomes to the trans-Golgi network and are a key part of the intracellular membrane network. This work reveals that the prototypic poxvirus vaccinia virus (VACV) exploits cellular retrograde transport pathways to facilitate the wrapping of intracellular mature virions and therefore promote the production of extracellular virus. Inhibition of retrograde transport by small-molecule inhibitors reduced the replication of VACV in cell culture and alleviated disease in mice experimentally infected with VACV. This research provides fundamental new knowledge about the wrapping step of poxvirus morphogenesis, furthers our knowledge of the complex cellular retrograde pathways, and identifies a new group of antipoxvirus drugs.

Grants and funding

This work was supported by strategic program grants BBS/E/D/20241864 and BBS/E/D/20241866 from the BBSRC to P.M.B. and P.D. and a University of Edinburgh Principal's Career Development Ph.D. Scholarship to K.H. Financial support was also provided by the Joint Ministerial Program of R&D against CBRNE risks, ANR grant Anti-HUS ANR-14-CE16-0004, Lermit LabEx grant R3 RetroLeishma, Ile de France Region grant from the DIM Malinf Initiative 140101, and CEA.