PLoS Pathogens (Jan 2013)

Nodular inflammatory foci are sites of T cell priming and control of murine cytomegalovirus infection in the neonatal lung.

  • Felix R Stahl,
  • Katrin Heller,
  • Stephan Halle,
  • Kirsten A Keyser,
  • Andreas Busche,
  • Anja Marquardt,
  • Karen Wagner,
  • Jasmin Boelter,
  • Yvonne Bischoff,
  • Elisabeth Kremmer,
  • Ramon Arens,
  • Martin Messerle,
  • Reinhold Förster

DOI
https://doi.org/10.1371/journal.ppat.1003828
Journal volume & issue
Vol. 9, no. 12
p. e1003828

Abstract

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Neonates, including mice and humans, are highly susceptible to cytomegalovirus (CMV) infection. However, many aspects of neonatal CMV infections such as viral cell tropism, spatio-temporal distribution of the pathogen as well as genesis of antiviral immunity are unknown. With the use of reporter mutants of the murine cytomegalovirus (MCMV) we identified the lung as a primary target of mucosal infection in neonatal mice. Comparative analysis of neonatal and adult mice revealed a delayed control of virus replication in the neonatal lung mucosa explaining the pronounced systemic infection and disease in neonates. This phenomenon was supplemented by a delayed expansion of CD8(+) T cell clones recognizing the viral protein M45 in neonates. We detected viral infection at the single-cell level and observed myeloid cells forming "nodular inflammatory foci" (NIF) in the neonatal lung. Co-localization of infected cells within NIFs was associated with their disruption and clearance of the infection. By 2-photon microscopy, we characterized how neonatal antigen-presenting cells (APC) interacted with T cells and induced mature adaptive immune responses within such NIFs. We thus define NIFs of the neonatal lung as niches for prolonged MCMV replication and T cell priming but also as sites of infection control.