Herpes Virus Reshapes Human DNA, Opening Door for Novel Antiviral Strategies

July 4, 2025
Herpes Virus Reshapes Human DNA, Opening Door for Novel Antiviral Strategies
  • A recent study published in Nature Communications reveals that the herpes simplex virus-1 (HSV-1) can rearrange the DNA structure in human cells shortly after infection, allowing it to access essential host genes more effectively.

  • Dr. Esther González Almela, the first author of the study, describes HSV-1 as an 'opportunistic interior designer' that manipulates the human genome to exploit host resources for its replication.

  • Blocking the enzyme topoisomerase I in the host cell prevents HSV-1 from rearranging the host genome and stops the production of new viral particles, highlighting potential avenues for antiviral development.

  • The complete inhibition of TOP1 expression halted HSV-1 infection, although current TOP inhibitors do not specifically target the virus.

  • Researchers utilized advanced imaging techniques to observe significant changes in cellular DNA within just eight hours of HSV-1 infection, demonstrating that the virus alters the shape and compactness of host chromosomes.

  • By the third hour of infection, HSV-1 had utilized topoisomerase I and cohesin, leading to a 30% compaction of the DNA's volume and a notable reduction in the transcription of human genes.

  • Within the first hour of infection, HSV-1 co-opts key host genes, including RNA polymerase II and DNA topoisomerase, which contribute to the condensation of the host's chromatin into dense bundles.

  • The microscopy technique STORM-PAINT used in this research allows for high-resolution imaging of DNA molecules, enhancing our understanding of how viruses manipulate host chromatin.

  • This research could pave the way for new treatments targeting HSV-1 infections, which affect a significant portion of the population.

  • Approximately two-thirds of individuals are estimated to carry HSV-1, often asymptomatically, but it can lead to serious complications such as cold sores and blindness in vulnerable populations.

  • The findings raise new questions about the relationship between chromatin organization and function, with implications for understanding both viral strategies and the complexities of the human genome.

  • This study challenges previous assumptions that dense chromatin solely shuts down genes, suggesting a more intricate relationship between transcription activity and DNA structure.

Summary based on 2 sources


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