DbpA, but Not OspA, Is Expressed by Borrelia burgdorferi during Spirochetemia and Is a Target for Protective Antibodies

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Infection and Immunity, November 1998, p. 5379-5387, Vol. 66, No. 11
0019-9567/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

DbpA, but Not OspA, Is Expressed by Borrelia burgdorferi during Spirochetemia and Is a Target for Protective Antibodies

David R. Cassatt,^* Nita K. Patel, Nancy D. Ulbrandt, and Mark S. Hanson

MedImmune, Inc., Gaithersburg, Maryland 20878

Received 29 June 1998/Returned for modification 11 August 1998/Accepted 28 August 1998

DbpA is a target for antibodies that protect mice against infection by cultured Borrelia burgdorferi. Infected mice exhibitearly and sustained humoral responses to DbpA and DbpB, suggestingthat these proteins are expressed in vivo. Many antigens expressedin mammals by B. burgdorferi are repressed in vitro at lower growthtemperatures, and we have now extended these observations to includeDbpA and DbpB. To confirm that the protective antigen DbpA isexpressed in vivo and to address the question of its accessibilityto antibodies during infection, we examined B. burgdorferi inblood samples from mice following cutaneous inoculation. B. burgdorferiwas visualized by dark-field microscopy in plasma samples fromspirochetemic mice, and an indirect immunofluorescence assay showedthat these spirochetes were DbpA positive and OspA negative. Wedeveloped an ex vivo borreliacidal assay to show that hyperimmuneantiserum against DbpA, but not OspA, killed these plasma-derivedspirochetes, demonstrating that DbpA is accessible to antibodiesduring this phase of infection. Blood transferred from spirochetemicdonor mice readily established B. burgdorferi infection in naiverecipient mice or mice hyperimmunized with OspA, while mice hyperimmunizedwith DbpA showed significant protection against challenge withhost-adapted spirochetes. Antiserum from persistently infectedmice had borreliacidal activity against both cultured and plasma-derivedspirochetes, and adsorption of this serum with DbpA substantiallydepleted this killing activity. Our observations show that immunizationwith DbpA blocks B. burgdorferi dissemination from the site ofcutaneous inoculation and suggest that DbpA antibodies may contributeto control of persistent infection.

^* Corresponding author. Mailing address: MedImmune, Inc., 35 West Watkins Mill Rd., Gaithersburg, MD 20878. Phone: (301) 527-4308.Fax: (301) 527-4200. E-mail: cassattd{at}medimmune.com.

Infection and Immunity, November 1998, p. 5379-5387, Vol. 66, No. 11
0019-9567/98/$04.00+0
Copyright © 1998, American Society for Microbiology. All rights reserved.

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