The large tegument protein pUL36 is essential for formation of the capsid vertex-specific component at the capsid-tegument interface of herpes simplex virus 1.

Wan H Fan,Marion Mcelwee,David Bhella,Frazer J Rixon,Ashley P E Roberts,Rebecca Lauder,L Hutt-Fletcher

doi:10.1128/jvi.02887-14

Abstract

ABSTRACTHerpesviruses have a characteristic particle structure comprising an icosahedral capsid, which contains the DNA genome and is, in turn, surrounded by a proteinaceous tegument layer and a lipid envelope. In herpes simplex virus, the interaction between the capsid and tegument is limited to the capsid vertices and involves two minor capsid proteins, pUL17 and pUL25, and the large inner tegument protein pUL36. pUL17 and pUL25 form a heterodimeric structure, the capsid vertex-specific component (CVSC), that lies on top of the peripentonal triplexes, while pUL36 has been reported to connect the CVSC to the penton. In this study, we used virus mutants with deletions in the genes for pUL36 and another inner tegument protein, pUL37, to analyze the contributions of these proteins to CVSC structure. Using electron cryomicroscopy and icosahedral reconstruction of mutants that express pUL17 and pUL25 but not pUL36, we showed that in contrast to accepted models, the CVSC is not formed from pUL17 and pUL25 on their own but requires a contribution from pUL36. In addition, the presence of full-length pUL36 results in weak density that extends the CVSC toward the penton, suggesting either that this extra density is formed directly by pUL36 or that pUL36 stabilizes other components of the vertex-tegument interface. IMPORTANCE Herpesviruses have complex particles that are formed as a result of a carefully controlled sequence of assembly steps. The nature of the interaction between two of the major particle compartments, the icosahedral capsid and the amorphous tegument, has been extensively studied, but the identity of the interacting proteins and their roles in forming the connections are still unclear. In this study, we used electron microscopy and three-dimensional reconstruction to analyze virus particles formed by mutants that do not express particular interacting proteins. We show that the largest viral protein, pUL36, which occupies the layer of tegument closest to the capsid, is essential for formation of structurally normal connections to the capsid. This demonstrates the importance of pUL36 in the initial stages of tegument addition and provides new insights into the process of virus particle assembly.

Highlights

Herpesviruses have a characteristic particle structure comprising an icosahedral capsid, which contains the DNA genome and is, in turn, surrounded by a proteinaceous tegument layer and a lipid envelope
High-resolution reconstruction of mature gammaherpesvirus (Kaposi’s sarcoma-associated herpesvirus [KSHV]) virions has produced a different interpretation by revealing that the distal part of the archetypal capsid vertex-specific component (CVSC) that sits above the two triplexes (Ta and Tc in reference 41) is formed by the KSHV homologue of pUL17, with the pUL25 homologue occupying a position on top of the penton [35]
To analyze the sequence of events occurring during tegument addition, we determined the structures of cytoplasmic C-capsids prepared from BHK cells infected with wildtype (WT) herpes simplex virus type 1 (HSV-1) and two inner tegument mutants with complete deletions of the UL36 (AR⌬UL36) and UL37 (FR⌬UL37) genes [20]

Summary

Introduction

Herpesviruses have a characteristic particle structure comprising an icosahedral capsid, which contains the DNA genome and is, in turn, surrounded by a proteinaceous tegument layer and a lipid envelope. We show that the largest viral protein, pUL36, which occupies the layer of tegument closest to the capsid, is essential for formation of structurally normal connections to the capsid This demonstrates the importance of pUL36 in the initial stages of tegument addition and provides new insights into the process of virus particle assembly. High-resolution reconstruction of mature gammaherpesvirus (Kaposi’s sarcoma-associated herpesvirus [KSHV]) virions has produced a different interpretation by revealing that the distal part of the archetypal CVSC that sits above the two triplexes (Ta and Tc in reference 41) is formed by the KSHV homologue of pUL17, with the pUL25 homologue occupying a position on top of the penton [35] This essentially inverts the positions of these two proteins from those proposed in the earlier studies

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