Cell Reports (Jan 2017)

A Systems Approach Reveals MAVS Signaling in Myeloid Cells as Critical for Resistance to Ebola Virus in Murine Models of Infection

  • Mukta Dutta,
  • Shelly J. Robertson,
  • Atsushi Okumura,
  • Dana P. Scott,
  • Jean Chang,
  • Jeffrey M. Weiss,
  • Gail L. Sturdevant,
  • Friederike Feldmann,
  • Elaine Haddock,
  • Abhilash I. Chiramel,
  • Sanket S. Ponia,
  • Jonathan D. Dougherty,
  • Michael G. Katze,
  • Angela L. Rasmussen,
  • Sonja M. Best

DOI
https://doi.org/10.1016/j.celrep.2016.12.069
Journal volume & issue
Vol. 18, no. 3
pp. 816 – 829

Abstract

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The unprecedented 2013–2016 outbreak of Ebola virus (EBOV) resulted in over 11,300 human deaths. Host resistance to RNA viruses requires RIG-I-like receptor (RLR) signaling through the adaptor protein, mitochondrial antiviral signaling protein (MAVS), but the role of RLR-MAVS in orchestrating anti-EBOV responses in vivo is not known. Here we apply a systems approach to MAVS−/− mice infected with either wild-type or mouse-adapted EBOV. MAVS controlled EBOV replication through the expression of IFNα, regulation of inflammatory responses in the spleen, and prevention of cell death in the liver, with macrophages implicated as a major cell type influencing host resistance. A dominant role for RLR signaling in macrophages was confirmed following conditional MAVS deletion in LysM+ myeloid cells. These findings reveal tissue-specific MAVS-dependent transcriptional pathways associated with resistance to EBOV, and they demonstrate that EBOV adaptation to cause disease in mice involves changes in two distinct events, RLR-MAVS antagonism and suppression of RLR-independent IFN-I responses.

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