Your search keyword '"Maedi"' showing total 2 results

1. Perivascular inflammatory cells in ovine Visna/maedi encephalitis and their possible role in virus infection and lesion progression.

Author

Polledo, Laura, González, Jorge, Benavides, Julio, Martínez-Fernández, Beatriz, Ferreras, Ma., and Marín, Juan

Subjects

*LENTIVIRUS diseases, *CELLS, *INFLAMMATION, *DISEASE progression, *ANTIGENS, *T cells, *LYMPHOCYTES, *IMMUNOHISTOCHEMISTRY

Abstract

We examined the distribution in the perivascular spaces of Visna/maedi antigen, T cells (CD3+, CD4+ and CD8+), B cells and macrophages by immunohistochemistry in 22 natural cases of Visna/maedi encephalitis. Sheep showed lymphocytic or histiocytic lesions. In mild lymphocytic lesions, the viral antigen was detected in perivascular cuffs where CD8+ T cells predominated, but in severe lymphocytic lesions, sparse antigen was identified, and CD8+/CD4+ T cells appeared in a similar proportion in multilayer perivascular sleeves. In histiocytic lesions, vessels were surrounded by macrophages with abundant viral antigen, with CD8+/CD4+ T cells and B cells in the periphery. These results could reflect different stages of virus neuroinvasion and clarify the neuropathogenesis of Visna/maedi encephalitis. [ABSTRACT FROM AUTHOR]

Published

2012

2. Vaccination delays maedi-visna lentivirus infection in a naturally-infected sheep flock

Author

Margrét Gudnadóttir, Andreas Demosthenous, and Theophanis Hadjisavvas

Subjects

Vaccine-trial, Visna-maedi virus, viruses, Blotting, Western, Antibodies, Viral, Challenge by natural infection, Virus, Visna, Animals, Maedi-Visna, Maedi, lcsh:Veterinary medicine, Sheep, General Veterinary, biology, Viral Vaccine, Lentivirus, Vaccine trial, Viral Vaccines, General Medicine, biology.organism_classification, Virology, Antibodies, Neutralizing, veterinary(all), Vaccination, Immunology, Antibody Formation, biology.protein, Disease Progression, lcsh:SF600-1100, Female, Antibody, Research Article

Abstract

Background The Maedi-Visna (MV) lentivirus causes two slowly progressive eventually fatal diseases of sheep, Maedi, a progressive interstitial pneumonia, and Visna, a progressive demyelinating disease of the central nervous system. Other lentiviruses also cause fatal slow infections in their natural hosts, e.g. the HIV virus in humans. Results of experimental vaccination against any lentivirus where vaccinees are challenged by natural routes, may therefore be of general interest. From 1991–1998 experiments with formalin-inactivated whole Maedi-Visna virus vaccine were carried out in the Department of Microbiology at the University of Iceland. Western Blot tests showed good immune response to all major proteins of the virus. When aluminium hydroxide was added to the vaccine all vaccinees developed neutralizing antibodies to the vaccine strain at titers 1/8 – 1/256. After housing 5 twin pairs, one twin in each pair vaccinated, the other unvaccinated, with infected sheep for 4 years, all the unvaccinated twins became infected, but only 2 of their vaccinated siblings as confirmed by virus cultivation experiments on tissues from their lungs spleens lymph nodes and choroid plexuses. Results One twin in each of 40 female twin pairs, born into a Maedi-Visna-infected sheep flock and kept under natural farming conditions in Cyprus, was vaccinated at birth, 3 weeks and 3 months, with formalin-inactivated whole Maedi-Visna lentivirus vaccine adjuvanted with aluminium hydroxide. 17 mothers of the twins were seronegative, 13 seroconverting and 10 had old infection. Of 17 vaccinees born to seronegative mothers 9 were uninfected at 28 months, but only 2 of their unvaccinated siblings. Of 13 unvaccinated twins born to seroconverting mothers, 12 caught infection during their first 10 weeks, but only 4 of their vaccinated siblings. Vaccination had no effects on 10 vaccinees born to mothers with long-standing Maedi-Visna infections and broad andibody response at birth of their lambs. Conclusion Compared with their unvaccinated siblings, natural infection was delayed in significant number of vaccinated twins born by seronegative and seroconverting mothers and vaccinated at birth, 3 weeks and 3 months with formalin inactivated whole MV vaccine adjuvanted with aluminium hydroxide. Maternal antibodies interfered with vaccination so early in life if the mother had old infection.