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  4. Therapeutic passive vaccination against chronic Lyme disease in mice

Therapeutic passive vaccination against chronic Lyme disease in mice

Author(s)
Zhong, Weimin
Stehle, Thomas
Museteanu, Crisan
Siebers, Annette
Gern, Lise  
Poste de physiologie comportementale  
Kramer, Michael
Wallich, Reinhard
Simon, Markus M
Date issued
1997
In
Proceedings of the National Academy of Sciences of the United States of America
Vol
23
No
94
From page
12533
To page
12538
Subjects
OUTER SURFACE-PROTEIN BORRELIA-BURGDORFERI INFECTION IMMUNODEFICIENCY SCID MOUSE TREATMENT-RESISTANT MONOCLONAL-ANTIBODIES PROTECTIVE IMMUNITY RECOMBINANT OSPA ARTHRITIS PERSISTENCE STRAINS
Abstract
Passive and active immunization against outer surface protein A (OspA) has been successful in protecting laboratory animals against subsequent infection with Borrelia burgdorferi. Antibodies (Abs) to OspA convey full protection, but only when they are present at the time of infection, Abs inactivate spirochetes within the tick and block their transmission to mammals, but do not affect established infection because of the loss of OspA in the vertebrate host. Our initial finding that the presence of high serum titers of anti-OspC Abs (5 to 10 mu g/ml) correlates with spontaneous resolution of disease and infection in experimentally challenged immunocompetent mice suggested that therapeutic vaccination with OspC may be feasible. We now show that polyclonal and monospecific mouse immune sera to recombinant OspC, but not to OspA, of B. burgdorferi resolve chronic arthritis and carditis and clear disseminated spirochetes in experimentally infected C.B.-17 severe combined immunodeficient mice in a dose-dependent manner. This was verified by macroscopical and microscopical examination of affected tissues and recultivation of spirochetes from ear biopsies. Complete resolution of disease and infection was achieved, independent of whether OspC-specific immune sera (10 mu g OspC-specific Abs) were repeatedly given (4 x in 3- to 4-day intervals) before the onset (day 10 postinfection) or at the time of fully established arthritis and carditis (days 19 or 60 postinfection). The results indicate that in mice spirochetes constitutively express OspC and are readily susceptible to protective OspC-specific Abs throughout the infection. Thus, an OspC-based vaccine appears to be a candidate for therapy of Lyme disease.
Publication type
journal article
Identifiers
https://libra.unine.ch/handle/20.500.14713/50897
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