Frontiers in Immunology (Jun 2021)

Activation of the Anti-Oxidative Stress Response Reactivates Latent HIV-1 Through the Mitochondrial Antiviral Signaling Protein Isoform MiniMAVS

  • Indra Sarabia,
  • Camille L. Novis,
  • Amanda B. Macedo,
  • Hiroshi Takata,
  • Racheal Nell,
  • Juyeon C. Kakazu,
  • Robert L. Furler,
  • Binita Shakya,
  • Heidi L. Schubert,
  • Christopher P. Hill,
  • Ana Beatriz DePaula-Silva,
  • Adam M. Spivak,
  • Lydie Trautmann,
  • Vicente Planelles,
  • Alberto Bosque

DOI
https://doi.org/10.3389/fimmu.2021.682182
Journal volume & issue
Vol. 12

Abstract

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The mitochondrial antiviral signaling protein (MAVS) is part of the cell’s innate immune mechanism of defense. MAVS mRNA is bicistronic and can give rise to a full length-MAVS and a shorter isoform termed miniMAVS. In response to viral infections, viral RNA can be sensed by the cytosolic RNA sensors retinoic acid-inducible gene I (RIG-I) and/or melanoma differentiation-associated protein 5 (MDA5) and activate NF-κB through interaction with MAVS. MAVS can also sense cellular stress and activate an anti-oxidative stress (AOS) response through the activation of NF-κB. Because NF-κB is a main cellular transcription factor for HIV-1, we wanted to address what role MAVS plays in HIV-1 reactivation from latency in CD4 T cells. Our results indicate that RIG-I agonists required full length-MAVS whereas the AOS response induced by Dynasore through its catechol group can reactivate latent HIV-1 in a MAVS dependent manner through miniMAVS isoform. Furthermore, we uncover that PKC agonists, a class of latency-reversing agents, induce an AOS response in CD4 T cells and require miniMAVS to fully reactivate latent HIV-1. Our results indicate that the AOS response, through miniMAVS, can induce HIV-1 transcription in response to cellular stress and targeting this pathway adds to the repertoire of approaches to reactivate latent HIV-1 in ‘shock-and-kill’ strategies.

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