Molecular cloning and host range analysis of three cytomegaloviruses from Mastomys natalensis
Laura Staliunaite, Olha Puhach, Eleonore Ostermann, Kyle Rosenke, Jenna Nichols, Lisa Oestereich, Nafomon Sogoba, Heinz Feldmann, Andrew J. Davison, Michael A. Jarvis, Wolfram Brune

TL;DR
This paper explores the potential of cytomegaloviruses from a rodent species as vaccine vectors to combat a deadly human virus.
Contribution
The study successfully cloned three MnatCMV genomes and identified a site for inserting vaccine antigens.
Findings
Three complete MnatCMV genomes were cloned using a YAC-BAC hybrid vector.
MnatCMVs showed a narrow host range, replicating only in M. natalensis cells.
A transgene insertion site was identified in MnatCMV2 suitable for vaccine antigen incorporation.
Abstract
Herpesvirus-based vectors are attractive for use as conventional or transmissible vaccines against emerging zoonoses in inaccessible animal populations. In both cases, cytomegaloviruses (CMVs) as members of the subfamily Betaherpesvirinae are particularly suitable for vaccine development as they are highly specific for their natural host species, infect a large proportion of their host population, and cause mild infections in healthy individuals. The Natal multimammate mouse (Mastomys natalensis) is the natural reservoir of Lassa virus, which causes deadly hemorrhagic fever in humans. M. natalensis was recently reported to harbor at least three different cytomegaloviruses (MnatCMV1, MnatCMV2, and MnatCMV3). Herein, we report the molecular cloning of three complete MnatCMV genomes in a yeast and bacterial artificial chromosome (YAC-BAC) hybrid vector. Purified viral genomes were cloned…
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Taxonomy
TopicsCytomegalovirus and herpesvirus research · Herpesvirus Infections and Treatments · Mosquito-borne diseases and control
