PLoS Pathogens (Jan 2013)

Absence of Siglec-H in MCMV infection elevates interferon alpha production but does not enhance viral clearance.

  • Franz Puttur,
  • Catharina Arnold-Schrauf,
  • Katharina Lahl,
  • Gulhas Solmaz,
  • Marc Lindenberg,
  • Christian Thomas Mayer,
  • Melanie Gohmert,
  • Maxine Swallow,
  • Christopher van Helt,
  • Heike Schmitt,
  • Lars Nitschke,
  • Bart N Lambrecht,
  • Roland Lang,
  • Martin Messerle,
  • Tim Sparwasser

DOI
https://doi.org/10.1371/journal.ppat.1003648
Journal volume & issue
Vol. 9, no. 9
p. e1003648

Abstract

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Plasmacytoid dendritic cells (pDCs) express the I-type lectin receptor Siglec-H and produce interferon α (IFNα), a critical anti-viral cytokine during the acute phase of murine cytomegalovirus (MCMV) infection. The ligands and biological functions of Siglec-H still remain incompletely defined in vivo. Thus, we generated a novel bacterial artificial chromosome (BAC)-transgenic "pDCre" mouse which expresses Cre recombinase under the control of the Siglec-H promoter. By crossing these mice with a Rosa26 reporter strain, a representative fraction of Siglec-H⁺ pDCs is terminally labeled with red fluorescent protein (RFP). Interestingly, systemic MCMV infection of these mice causes the downregulation of Siglec-H surface expression. This decline occurs in a TLR9- and MyD88-dependent manner. To elucidate the functional role of Siglec-H during MCMV infection, we utilized a novel Siglec-H deficient mouse strain. In the absence of Siglec-H, the low infection rate of pDCs with MCMV remained unchanged, and pDC activation was still intact. Strikingly, Siglec-H deficiency induced a significant increase in serum IFNα levels following systemic MCMV infection. Although Siglec-H modulates anti-viral IFNα production, the control of viral replication was unchanged in vivo. The novel mouse models will be valuable to shed further light on pDC biology in future studies.