Cell Reports (Jul 2017)

DDX6 Represses Aberrant Activation of Interferon-Stimulated Genes

  • Jennifer H. Lumb,
  • Qin Li,
  • Lauren M. Popov,
  • Siyuan Ding,
  • Marie T. Keith,
  • Bryan D. Merrill,
  • Harry B. Greenberg,
  • Jin Billy Li,
  • Jan E. Carette

DOI
https://doi.org/10.1016/j.celrep.2017.06.085
Journal volume & issue
Vol. 20, no. 4
pp. 819 – 831

Abstract

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The innate immune system tightly regulates activation of interferon-stimulated genes (ISGs) to avoid inappropriate expression. Pathological ISG activation resulting from aberrant nucleic acid metabolism has been implicated in autoimmune disease; however, the mechanisms governing ISG suppression are unknown. Through a genome-wide genetic screen, we identified DEAD-box helicase 6 (DDX6) as a suppressor of ISGs. Genetic ablation of DDX6 induced global upregulation of ISGs and other immune genes. ISG upregulation proved cell intrinsic, imposing an antiviral state and making cells refractory to divergent families of RNA viruses. Epistatic analysis revealed that ISG activation could not be overcome by deletion of canonical RNA sensors. However, DDX6 deficiency was suppressed by disrupting LSM1, a core component of mRNA degradation machinery, suggesting that dysregulation of RNA processing underlies ISG activation in the DDX6 mutant. DDX6 is distinct among DExD/H helicases that regulate the antiviral response in its singular ability to negatively regulate immunity.

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