PLoS Pathogens (Nov 2020)

Ifit2 deficiency restricts microglial activation and leukocyte migration following murine coronavirus (m-CoV) CNS infection.

  • Jayasri Das Sarma,
  • Amy Burrows,
  • Patricia Rayman,
  • Mi-Hyun Hwang,
  • Soumya Kundu,
  • Nikhil Sharma,
  • Cornelia Bergmann,
  • Ganes C Sen

DOI
https://doi.org/10.1371/journal.ppat.1009034
Journal volume & issue
Vol. 16, no. 11
p. e1009034

Abstract

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The interferon-induced tetratricopeptide repeat protein (Ifit2) protects mice from lethal neurotropic viruses. Neurotropic coronavirus MHV-RSA59 infection of Ifit2-/- mice caused pronounced morbidity and mortality accompanied by rampant virus replication and spread throughout the brain. In spite of the higher virus load, induction of many cytokines and chemokines in the brains of infected Ifit2-/- mice were similar to that in wild-type mice. In contrast, infected Ifit2-/- mice revealed significantly impaired microglial activation as well as reduced recruitment of NK1.1 T cells and CD4 T cells to the brain, possibly contributing to the lack of viral clearance. These two deficiencies were associated with a lower level of microglial expression of CX3CR1, the receptor of the CX3CL1 (Fractalkine) chemokine, which plays a critical role in both microglial activation and leukocyte recruitment. The above results uncovered a new potential role of an interferon-induced protein in immune protection.