Protective effect of surfactant protein D in pulmonary vaccinia virus infection: Implication of A27 viral protein

Julien Perino, Nicole M. Thielens, Erika Crouch, Danièle Spehner, Jean Marc Crance, Anne Laure Favier

Research output: Contribution to journalArticlepeer-review

11 Scopus citations

Abstract

Vaccinia virus (VACV) was used as a surrogate of variola virus (VARV) (genus Orthopoxvirus), the causative agent of smallpox, to study Orthopoxvirus infection. VARV is principally transmitted between humans by aerosol droplets. Once inhaled, VARV first infects the respiratory tract where it could encounter surfactant components, such as soluble pattern recognition receptors. Surfactant protein D (SP-D), constitutively present in the lining fluids of the respiratory tract, plays important roles in innate host defense against virus infection. We investigated the role of SP-D in VACV infection and studied the A27 viral protein involvement in the interaction with SP-D. Interaction between SP-D and VACV caused viral inhibition in a lung cell model. Interaction of SP-D with VACV was mediated by the A27 viral protein. Binding required Ca2+ and interactions were blocked in the presence of excess of SP-D saccharide ligands. A27, which lacks glycosylation, directly interacted with SP-D. The interaction between SP-D and the viral particle was also observed using electron microscopy. Infection of mice lacking SP-D (SP-D-/-) resulted in increased mortality compared to SP-D+/+ mice. Altogether, our data show that SP-D participates in host defense against the vaccinia virus infection and that the interaction occurs with the viral surface protein A27.

Original languageEnglish
Pages (from-to)928-953
Number of pages26
JournalViruses
Volume5
Issue number3
DOIs
StatePublished - Mar 21 2013

Keywords

  • A27 protein
  • Ca
  • Innate immunity
  • KO mice
  • Orthopoxvirus
  • Pulmonary infection
  • Sugars
  • Surfactant protein A
  • Surfactant protein D
  • Vaccinia virus

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