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J. Virol., 01 1998, 320-329, Vol 72, No. 1
H Deng and S Dewhurst
Sequences present at the genomic termini of herpesviruses become linked
during lytic-phase replication and provide the substrate for cleavage and
packaging of unit length viral genomes. We have previously shown that
homologs of the consensus herpesvirus cleavage-packaging signals, pac1 and
pac2, are located at the left and right genomic termini of human
herpesvirus 6 (HHV-6), respectively. Immediately adjacent to these elements
are two distinct arrays of human telomeric repeat sequences (TRS). We now
show that the unique sequence element formed at the junction of HHV-6B
genome concatemers (pac2-pac1) is necessary and sufficient for virally
mediated cleavage of plasmid DNAs containing the HHV-6B lytic-phase origin
of DNA replication (oriLyt). The concatemeric junction sequence also
allowed for the packaging of these plasmid molecules into intracellular
nucleocapsids as well as mature, infectious viral particles. In addition,
this element significantly enhanced the replication efficiency of
oriLyt-containing plasmids in virally infected cells. Experiments revealed
that the concatemeric junction sequence possesses an unusual, S1
nuclease-sensitive conformation (anisomorphic DNA), which might play a role
in this apparent enhancement of DNA replication--although additional
studies will be required to test this hypothesis. Finally, we also analyzed
whether the presence of flanking viral TRS had any effect on the functional
activity of the minimal concatemeric junction (pac2-pac1). These
experiments revealed that the TRS motifs, either alone or in combination,
had no effect on the efficiency of virally mediated DNA replication or DNA
cleavage. Taken together, these data show that the cleavage and packaging
of HHV-6 DNA are mediated by cis-acting consensus sequences similar to
those found in other herpesviruses, and that these sequences also influence
the efficiency of HHV-6 DNA replication. Since the adjacent TRS do not
influence either viral cleavage and packaging or viral DNA replication,
their function remains uncertain.
Copyright © 1998, American Society for Microbiology
Functional identification and analysis of cis-acting sequences which mediate genome cleavage and packaging in human herpesvirus 6
Department of Microbiology and Immunology, University of Rochester Medical Center, New York 14642, USA.
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