Back to Search Start Over

Splenic CD163+ macrophages as targets of porcine reproductive and respiratory virus Role of Siglecs

Authors :
Yuste, Miriam
Fernández-Caballero, T.
Prieto, Cinta
Álvarez, Belén
Martínez-Lobo, J.
Simarro, I.
Castro, Juan M.
Alonso, Fernando
Ezquerra Martínez, Ángel
Revilla Calvo, Concepción
Domínguez, Javier
Yuste, Miriam
Fernández-Caballero, T.
Prieto, Cinta
Álvarez, Belén
Martínez-Lobo, J.
Simarro, I.
Castro, Juan M.
Alonso, Fernando
Ezquerra Martínez, Ángel
Revilla Calvo, Concepción
Domínguez, Javier
Publication Year :
2017

Abstract

CD169 and CD163 have been involved in the process of PRRS virus attachment and infection in macrophages, although recent studies have challenged the requirement for CD169. In addition to CD169, macrophages express other siglecs, whose role in PRRS virus infection is so far unknown. Splenic CD163+ macrophages express Siglec-3 and Siglec-5 but almost undetectable levels of CD169. Hence, we considered this cell population appropriate for analysing the role of these siglecs in the attachment and internalization of PRRS virus into macrophages. PRRS virus replicated efficiently in these macrophages, yielding even higher titres than in alveolar macrophages. Besides, a recombinant protein consisting in the ectodomain of porcine Siglec-3 fused to the Fc fragment of human IgG1 (Siglec3-Fc) was able to bind PRRS virus, while binding to Siglec-5-Fc was inconsistent. Antibodies to CD169 but not to Siglec-3 or Siglec-5 blocked the binding and infection of PRRS virus on alveolar macrophages. Unexpectedly, our antibody to CD169 also blocked the binding of PRRS virus to splenic CD163+ macrophages, whereas antibodies to Siglec-3 or Siglec-5 had no effect. These results show that very low levels of CD169 expression are enough to support the attachment and internalization of PRRS virus into macrophages, whereas Siglec-3 and Siglec-5 do not seem to contribute to the virus entry in these cells.

Details

Database :
OAIster
Notes :
English
Publication Type :
Electronic Resource
Accession number :
edsoai.on1373153404
Document Type :
Electronic Resource