Litcius/Paper detail

c-Jun signaling during initial HSV-1 infection modulates latency to enhance later reactivation in addition to directly promoting the progression to full reactivation

Sara A. Dochnal, Abigail L. Whitford, Alison K. Francois, Patryk A. Krakowiak, Sean R. Cuddy, Anna R. Cliffe

2024Journal of Virology17 citationsDOIOpen Access PDF

Abstract

The molecular mechanisms that regulate the reactivation of herpes simplex virus-1 (HSV-1) from latent infection are unknown. The host transcription and pioneer factor c-Jun is the main target of the JNK cell stress pathway that is known to be important in exit of HSV from latency. Surprisingly, we found that c-Jun does not act with JNK during exit from latency but instead promotes the transition to full reactivation. Moreover, c-Jun and enhanced neuronal stress during initial neuronal infection promoted a more reactivation-competent form of HSV-1 latency. c-Jun, therefore, functions at multiple stages during HSV-1 latent infection of neurons to promote reactivation. Importantly, this study contributes to a growing body of evidence that de novo HSV-1 infection conditions can modulate latent infection and impact future reactivation events, raising important questions on the clinical impact of stress during initial HSV-1 acquisition on future reactivation events and consequences.

Topics & Concepts

BiologyHerpes simplex virusLatency (audio)Virus latencyVirologyImmunologyLatent VirusVirusTranscription factorCell biologyViral replicationGeneticsGeneElectrical engineeringEngineeringHerpesvirus Infections and TreatmentsToxin Mechanisms and ImmunotoxinsPoxvirus research and outbreaks