Frontiers in Cellular and Infection Microbiology (Nov 2021)

Proteome Profiling of RNF213 Depleted Cells Reveals Nitric Oxide Regulator DDAH1 Antilisterial Activity

  • Lia Martina,
  • Lia Martina,
  • Caroline Asselman,
  • Caroline Asselman,
  • Caroline Asselman,
  • Fabien Thery,
  • Fabien Thery,
  • Katie Boucher,
  • Katie Boucher,
  • Katie Boucher,
  • Louis Delhaye,
  • Louis Delhaye,
  • Louis Delhaye,
  • Louis Delhaye,
  • Teresa M. Maia,
  • Teresa M. Maia,
  • Teresa M. Maia,
  • Bart Dermaut,
  • Bart Dermaut,
  • Bart Dermaut,
  • Sven Eyckerman,
  • Sven Eyckerman,
  • Francis Impens,
  • Francis Impens,
  • Francis Impens

DOI
https://doi.org/10.3389/fcimb.2021.735416
Journal volume & issue
Vol. 11

Abstract

Read online

RNF213 is a large, poorly characterized interferon-induced protein. Mutations in RNF213 are associated with predisposition for Moyamoya disease (MMD), a rare cerebrovascular disorder. Recently, RNF213 was found to have broad antimicrobial activity in vitro and in vivo, yet the molecular mechanisms behind this function remain unclear. Using mass spectrometry-based proteomics and validation by real-time PCR we report here that knockdown of RNF213 leads to transcriptional upregulation of MVP and downregulation of CYR61, in line with reported pro- and anti-bacterial activities of these proteins. Knockdown of RNF213 also results in downregulation of DDAH1, which we discover to exert antimicrobial activity against Listeria monocytogenes infection. DDAH1 regulates production of nitric oxide (NO), a molecule with both vascular and antimicrobial effects. We show that NO production is reduced in macrophages from RNF213 KO mice, suggesting that RNF213 controls Listeria infection through regulation of DDAH1 transcription and production of NO. Our findings propose a potential mechanism for the antilisterial activity of RNF213 and highlight NO as a potential link between RNF213-mediated immune responses and the development of MMD.

Keywords