Abstract
Orf virus (ORFV) is the type species of the Parapoxvirus genus of the family Poxviridae and infects sheep and goats, often around the mouth, resulting in acute pustular skin lesions. ORFV encodes several secreted immunomodulators including a broad-spectrum chemokine binding protein (CBP). Chemokines are a large family of secreted chemotactic proteins that activate and regulate inflammation induced leukocyte recruitment to sites of infection. In this study we investigated the role of CBP in vivo in the context of ORFV infection of sheep. The CBP gene was deleted from ORFV strain NZ7 and infections of sheep used to investigate the effect of CBP on pathogenesis. Animals were either infected with the wild type (wt) virus, CBP-knockout virus or revertant strains. Sheep were infected by scarification on the wool-less area of the hind legs at various doses of virus. The deletion of the CBP gene severely attenuated the virus, as only few papules formed when animals were infected with the CBP-knock-out virus at the highest dose (107 p.f.u). In contrast, large pustular lesions formed on almost all animals infected with the wt and revertant strains at 107 p.f.u. The lesions for the CBP-knock-out virus resolved approximately 5–6 days p.i, at a dose of 107 pfu whereas in animals infected with the wt and revertants at this dose, lesions began to resolve at approximately 10 days p.i. Few pustules developed at the lowest dose of 103 p.f.u. for all viruses. Immunohistochemistry of biopsy skin-tissue from pustules showed that the CBP-knockout virus replicated in all animals at the highest dose and was localized to the skin epithelium while haematoxylin and eosin staining showed histological features of the CBP-knockout virus typical of the parent virus with acanthosis, elongated rete ridges and orthokeratotic hyperkeratosis. MHC-II immunohistochemistry analysis for monocytes and dendritic cells showed greater staining within the papillary dermis of the CBP-knock-out virus compared with the revertant viruses, however this was not the case with the wt where staining was similar. Our results show that the CBP gene encodes a secreted immunodulator that has a critical role in virulence and pathogenesis.
Highlights
Orf is a debilitating skin disease of sheep and goats and is transmissible to man (Fleming et al, 2015)
The chemokine binding protein (CBP) gene shows surprising variability within the Orf virus (ORFV) species with the strain NZ7 CBP showing only 78% identity to the strain NZ2 CBP at the amino acid level (Seet et al, 2003). These differences are partly due to three insertions in CBP protein encoded by ORFV strain NZ7 (CBPNZ7) making the gene 27 nts longer than CBPNZ2 with a predicted polypeptide of 32.193 kDa compared with 31.182 kDa
The chemokine binding specificity of CBPNZ7 was compared with CBPNZ2 over a broad range of chemokines that are produced during inflammation in skin and the constitutive chemokine CCL19
Summary
Orf is a debilitating skin disease of sheep and goats and is transmissible to man (Fleming et al, 2015). We hypothesized that the ORFV CBP disrupts chemokine gradients within the skin tissue of its host during infection and thereby sets up a blockade to inhibit the recruitment of leukocytes to the infected site. For these studies we used ORFV strain NZ7. We firstly characterized the chemokine binding properties of the purified CBP protein encoded by ORFV strain NZ7 (CBPNZ7) by ELISA and its effects on monocyte migration in response to specific chemokines in a chemotaxis assay and inflammatory cell trafficking using a murine skin inflammation model. Infection studies were carried out in sheep using the recombinant virus and the clinical pathology and host response compared with the parent strain
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