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Herpesviruses mimic zygotic genome activation to promote viral replication

Authors

  • E. Neugebauer
  • S. Walter
  • J. Tan
  • N. Drayman
  • V. Franke
  • M. van Gent
  • S. Pennisi
  • P. Veratti
  • K.S. Stein
  • I. Welker
  • S. Tay
  • G.M.G.M. Verjans
  • H.T.M. Timmers
  • A. Akalin
  • M. Landthaler
  • A. Ensser
  • E. Wyler
  • F. Full

Journal

  • Nature Communications

Citation

  • Nat Commun 16 (1): 710

Abstract

  • Zygotic genome activation (ZGA) is crucial for maternal to zygotic transition at the 2-8-cell stage in order to overcome silencing of genes and enable transcription from the zygotic genome. In humans, ZGA is induced by DUX4, a pioneer factor that drives expression of downstream germline-specific genes and retroelements. Here we show that herpesviruses from all subfamilies, papillomaviruses and Merkel cell polyomavirus actively induce DUX4 expression to promote viral transcription and replication. Analysis of single-cell sequencing data sets from patients shows that viral DUX4 activation is of relevance in vivo. Herpes-simplex virus 1 (HSV-1) immediate early proteins directly induce expression of DUX4 and its target genes, which mimics zygotic genome activation. Upon HSV-1 infection, DUX4 directly binds to the viral genome and promotes viral transcription. DUX4 is functionally required for infection, since genetic depletion by CRISPR/Cas9 as well as degradation of DUX4 by nanobody constructs abrogates HSV-1 replication. Our results show that DNA viruses including herpesviruses mimic an embryonic-like transcriptional program that prevents epigenetic silencing of the viral genome and facilitates herpesviral gene expression.


DOI

doi:10.1038/s41467-025-55928-5