Cytomegalovirus Generates Assembly Compartment in the Early Phase of Infection by Perturbation of Host-Cell Factors Recruitment at the Early Endosome/Endosomal Recycling Compartment/Trans-Golgi Interface

Pero Lučin; Natalia Jug Vučko; Ljerka Karleuša; Hana Mahmutefendić Lučin; Gordana Blagojević Zagorac; Berislav Lisnić; Valentino Pavišić; Marina Marcelić; Kristina Grabušić; Ilija Brizić; Silvija Lukanović Jurić

doi:10.3389/fcell.2020.563607

Cytomegalovirus Generates Assembly Compartment in the Early Phase of Infection by Perturbation of Host-Cell Factors Recruitment at the Early Endosome/Endosomal Recycling Compartment/Trans-Golgi Interface

Front Cell Dev Biol. 2020 Sep 11:8:563607. doi: 10.3389/fcell.2020.563607. eCollection 2020.

Affiliations

¹ Department of Physiology and Immunology, Faculty of Medicine, University of Rijeka, Rijeka, Croatia.
² University North, University Center Varaždin, Varaždin, Croatia.
³ Department of Histology and Embryology, Faculty of Medicine, University of Rijeka, Rijeka, Croatia.

Abstract

Beta-herpesviruses develop a unique structure within the infected cell known as an assembly compartment (AC). This structure, as large as the nucleus, is composed of host-cell-derived membranous elements. The biogenesis of the AC and its contribution to the final stages of beta-herpesvirus assembly are still unclear. In this study, we performed a spatial and temporal analysis of the AC in cells infected with murine CMV (MCMV), a member of the beta-herpesvirus family, using a panel of markers that characterize membranous organelle system. Out of 64 markers that were analyzed, 52 were cytosolic proteins that are recruited to membranes as components of membrane-shaping regulatory cascades. The analysis demonstrates that MCMV infection extensively reorganizes interface between early endosomes (EE), endosomal recycling compartment (ERC), and the trans-Golgi network (TGN), resulting in expansion of various EE-ERC-TGN intermediates that fill the broad area of the inner AC. These intermediates are displayed as over-recruitment of host-cell factors that control membrane flow at the EE-ERC-TGN interface. Most of the reorganization is accomplished in the early (E) phase of infection, indicating that the AC biogenesis is controlled by MCMV early genes. Although it is known that CMV infection affects the expression of a large number of host-cell factors that control membranous system, analysis of the host-cell transcriptome and protein expression in the E phase of infection demonstrated no sufficiently significant alteration in expression levels of analyzed markers. Thus, our study demonstrates that MCMV-encoded early phase function targets recruitment cascades of host cell-factors that control membranous flow at the EE-ERC-TGN interface in order to initiate the development of the AC.

Keywords: Rab cascades; Rab proteins; cytomegalovirus; endosomal recycling compartment; virion assembly compartment.