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The Epstein-Barr virus episome maneuvers between nuclear chromatin compartments during reactivation

Journal of Virology, ISSN: 1098-5514, Vol: 92, Issue: 3
2018
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Article Description

The human genome is structurally organized in three-dimensional space to facilitate functional partitioning of transcription. We learned that the latent episome of the human Epstein-Barr virus (EBV) preferentially associates with genepoor chromosomes and avoids gene-rich chromosomes. Kaposi's sarcoma-associated herpesvirus behaves similarly, but human papillomavirus does not. Contacts on the EBV side localize to OriP, the latent origin of replication. This genetic element and the EBNA1 protein that binds there are sufficient to reconstitute chromosome association preferences of the entire episome. Contacts on the human side localize to gene-poor and AT-rich regions of chromatin distant from transcription start sites. Upon reactivation from latency, however, the episome moves away from repressive heterochromatin and toward active euchromatin. Our work adds three-dimensional relocalization to the molecular events that occur during reactivation. Involvement of myriad interchromosomal associations also suggests a role for this type of longrange association in gene regulation.

Bibliographic Details

Stephanie A. Moquin; Sean Thomas; Sean Whalen; Alix Warburton; Samantha G. Fernandez; Alison A. McBride; Katherine S. Pollard; JJ L. Miranda; Jae U. Jung

American Society for Microbiology

Immunology and Microbiology; Agricultural and Biological Sciences

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