Selective recruitment of host factors by HSV-1 replication centers
Herpes simplex virus type 1 (HSV-1) enters productive infection after infecting epithelial cells, where it controls the host nucleus to make viral proteins, starts viral DNA synthesis and assembles infectious virions. In this process, replicating viral genomes are organized into replication centers...
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Veröffentlicht in: | Dōngwùxué yánjiū 2015-05, Vol.36 (3), p.142-151 |
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Sprache: | eng |
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Zusammenfassung: | Herpes simplex virus type 1 (HSV-1) enters productive infection after
infecting epithelial cells, where it controls the host nucleus to make
viral proteins, starts viral DNA synthesis and assembles infectious
virions. In this process, replicating viral genomes are organized into
replication centers to facilitate viral growth. HSV-1 is known to use
host factors, including host chromatin and host transcription
regulators, to transcribe its genes; however, the invading virus also
encounters host defense and stress responses to inhibit viral growth.
Recently, we found that HSV-1 replication centers recruit host factor
CTCF but exclude γH2A.X. Thus, HSV-1 replication centers may
selectively recruit cellular factors needed for viral growth, while
excluding host factors that are deleterious for viral transcription or
replication. Here we report that the viral replication centers
selectively excluded modified histone H3, including heterochromatin
mark H3K9me3, H3S10P and active chromatin mark H3K4me3, but not
unmodified H3. We found a dynamic association between the viral
replication centers and host RNA polymerase II. The centers also
recruited components of the DNA damage response pathway, including
53BP1, BRCA1 and host antiviral protein SP100. Importantly, we found
that ATM kinase was needed for the recruitment of CTCF to the viral
centers. These results suggest that the HSV-1 replication centers took
advantage of host signaling pathways to actively recruit or exclude
host factors to benefit viral growth. |
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ISSN: | 2095-8137 0254-5853 2095-8137 |