Pathogenicity of blood orf virus isolates in the development of dairy goat contagious pustular dermatitis

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Orf is a clinical manifestation of parapoxvirus infection often fatal in goats and sheep especially when they are under stress or influenced by unfavorable environment. This study investigated the pathogenicity of two Orf virus isolates (ORFV UPM1/14 and UPM2/14) and host response in mouse model by using different inoculation sites with/without prior exposure to dexamethasone. Treatments with dexamethasone served as an immunosuppressant that may mimic stress situation in affected animals. Groups of five mice were given intradermal injection of 0.2 mL of tissue culture infective dose 50 (TCID50) of UPM1/14 (Group 1) and UPM2/14 (Group 2) at the dorsum (Group 1A; Group 2A), ear pinna (Group 1B; Group 2B), and labial commissure (Group 1C; Group 2C). An inoculum 0.2 mL of UPM1/14 was administered to animals treated with dexamethasone (n=5; 5 mg/kg/day intraperitoneally) and nondexamethasone (n=5) groups at the dorsum, ear pinna, and labial commissure. No significant difference (p>0.05) was observed in the mean lesion scores among the groups of different inoculation sites or between dexamethasone-treated and nontreated groups. However, there was a significant difference (p<0.05) in the mean stratum thickness of affected skin following inoculation with UPM2/14 isolate at the ear pinna and labial commissure. Histopathology examination revealed keratosis, acanthosis, and ballooning degeneration in the skin of affected mice. Orf virus DNA was detected in the skin samples by targeting F1L and B2L virus-specific genes in polymerase chain reaction (PCR) assay. Intradermal inoculation with UPM1/14 or UPM2/14 isolate produced a mild skin lesion in mice, and there was no significant difference in orf disease manifestation despite variation of inoculation sites. Similarly, short-term dexamethasone administration gave no adverse effects on pathogenicity of orf virus isolates.


Contagious pustular dermatitis (orf) is an exanthemous disease affecting sheep and goats primarily. As a zoonotic infectious disease caused by parapoxvirus, orf should be managed not only in animals but also in humans. In this study, the typical orf clinical symptoms in goat and humans were observed. Human and goat samples were drawn. The Orf virus (orfv) was identified using an electron microscope, and PCR was used to amplify the target for B2L gene sequence. Molecular analysis of other B2L gene sequences downloaded from GenBank was performed by Mega4 soft. Results indicated that a 21-year old girl who worked in a goat farmcontacted orfv infection from infected goats directly. Eleven amino acid (AA) mutations were detected in the goat orfv transmitted to human orfv. Phylogenetic analysis showed that human orfv in this study was closely related genetically to FJ-SJ2 (KC568397), which was isolated from Fujian province 2012. The results facilitate the development of programs to control Orf virus infections not only in goats but also in humans.


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