Fc-Dependent Polyclonal Antibodies and Antibodies to Outer Membrane Proteins A and B, but Not to Lipopolysaccharide, Protect SCID Mice against Fatal Rickettsia conorii Infection

doi:10.1128/IAI.72.4.2222-2228.2004

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Infection and Immunity, April 2004, p. 2222-2228, Vol. 72, No. 4
0019-9567/04/$08.00+0 DOI: 10.1128/IAI.72.4.2222-2228.2004
Copyright © 2004, American Society for Microbiology. All Rights Reserved.

Fc-Dependent Polyclonal Antibodies and Antibodies to Outer Membrane Proteins A and B, but Not to Lipopolysaccharide, Protect SCID Mice against Fatal Rickettsia conorii Infection

Hui-Min Feng, Ted Whitworth, Juan P. Olano, Vsevolod L. Popov, and David H. Walker^*

Department of Pathology, University of Texas Medical Branch, Galveston, Texas

Received 11 August 2003/ Returned for modification 29 September 2003/ Accepted 9 December 2003

An emphasis on cellular immunity against Rickettsia has ledto neglect of analysis of the role of antibody. The availabilityof an excellent mouse model of spotted fever rickettsiosis enabledinvestigation of a potential role of antibody in immunity toRickettsia conorii. C3H severe combined immunodeficiency (SCID)mice were passively transfused with monoclonal antibodies againstrickettsial outer membrane protein A (OmpA), OmpB, or lipopolysaccharide(LPS), polyclonal anti-R. conorii serum, Fab fragments of polyclonalantiserum, or no antibodies and then challenged 48 h later with10 50% lethal doses (LD₅₀) of R. conorii. All mice that receivedmonoclonal antibodies against OmpA and two of four mice thatreceived monoclonal antibodies against OmpB or polyclonal antiserawere completely protected, but the recipients of anti-LPS antibodiesor the Fab fragments were not protected. Polyclonal antibodytreatment of C3H SCID mice that had been infected with 10 LD₅₀of R. conorii 4 or 5 days earlier prolonged the life of theinfected mice from 10.4 to 22.5 days and resulted in decreasedlevels of infectious rickettsiae in the spleen and liver 24and 48 h later. Treatment with protective antibodies resultedin the development of large aggregates of R. conorii antigensin splenic macrophages and intraphagolysosomal rickettsial deathand digestion. The kinetics of development of antibodies toR. conorii determined by immunoblotting revealed antibodiesto LPS on day 6 and antibodies to OmpA and OmpB on day 12, whenrecovery from the infection had already occurred. Antibodiesto particular epitopes of OmpA and OmpB may protect againstreinfection, but they may not play a key role in immunity againstprimary infection. Antibodies might be useful for treating infectionswith antibiotic-resistant organisms, and some B-cell epitopesshould be included in a subunit vaccine.

* Corresponding author. Mailing address: University of Texas Medical Branch, 301 University Blvd., Keiller Bldg., Galveston, TX 77555-0609. Phone: (409) 772-2856. Fax: (409) 772-1850. E-mail: dwalker{at}utmb.edu.

Editor: W. A. Petri, Jr.

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