Effect of Antibody on the Rickettsia-Host Cell Interaction

Abstract

A recent study demonstrated that polyclonal antibodies toRickettsia conoriiand monoclonal antibodies to outer membrane proteins A (OmpA) and B (OmpB) provided effective, Fc-dependent, passive immunity, even in severe combined immunodeficient mice with an established infection. In order to determine the mechanism of protection, mouse endothelial and macrophage-like cell lines were infected withR. conoriithat had been exposed to polyclonal antibodies, monoclonal antibodies to OmpA or OmpB, Fab fragments of the polyclonal antibodies, or normal serum or that were left untreated. At 0 h, Fc-dependent antibody enhancement ofR. conoriiadherence to endothelial and macrophage-like cell lines was inhibited by the presence of normal serum, suggesting Fc receptor-mediated adherence of opsonized rickettsiae. At 3 h, the opsonized rickettsiae had been internalized. After 72 h, inhibited survival of rickettsiae exposed to polyclonal antibodies or monoclonal antibodies to OmpA or OmpB was evident compared with growth of untreated and normal serum-treated and polyclonal Fab antibody-treatedR. conorii. Polyclonal antibodies and an anti-OmpB monoclonal antibody inhibited the escape ofR. conoriifrom the phagosome, resulting in intraphagolysosomal rickettsial death. At 48 h of infection, rickettsicidal activity of macrophages by opsonized rickettsiae was inhibited by N^G-monomethyl-l-arginine, superoxide dismutase, mannitol, or supplementall-tryptophan, and endothelial rickettsicidal activity against opsonized rickettsiae was inhibited by N^G-monomethyl-l-arginine, superoxide dismutase, catalase, or supplementall-tryptophan. Thus, Fc-dependent antibodies protected againstR. conoriiinfection of endothelium and macrophages by opsonization that inhibited phagosomal escape and resulted in phagolysosomal killing mediated by nitric oxide, reactive oxygen intermediates, andl-tryptophan starvation.